Genetically engineered phiC31-integrase genes

ABSTRACT

Genetically engineered nucleic acid molecules encoding phiC31-integrase are described. These nucleic acid molecules, referred to as C31-Int genes, comprise sequences optimized for expression in eukaryotic host cells. Vectors, microorganisms, vertebrate cells, and transgenic organisms comprising optimized C31-Int genes are also described. PhiC31 integrase proteins encoded by the optimized C31-Int genes, as well as methods of recombining a DNA molecules containing phiC31 integrase recognition sequences are provided.

REFERENCE TO RELATED APPLICATIONS

[0001] This application claims priority to U.S. provisional patent application No. 60/354,741 filed Feb. 6, 2002. The contents of the prior application is hereby incorporated in its entirety.

BACKGROUND OF THE INVENTION

[0002] The ability to generate controlled and permanent modifications to genomes of eukaryotic cells and organisms has important research applications, including the study of gene function, the creation of disease models, medical applications such as gene therapy, and the design of economically important animals and crops.

[0003] Site-specific recombinases (SSRs), such as the bacteriophage P1-derived Cre recombinase, provide important tools for engineering eukaryotic genomes. SSRs recognize specific DNA sequences (“recognition sites” or “recognition sequences”) and catalyze recombination between two recognition sites. Cre recombinase, for example, recognizes the 34 base pair (bp) loxP motif (Austin et al., Cell 25, 729-736 (1981)). If the two sites are located on the same DNA molecule in the same orientation, the intervening DNA sequence is excised by the recombinase from the parental molecule as a closed circle, leaving one recognition site on each of the reaction products. If the two sites are in inverted orientation, the recognition-site flanked region is inverted through recombinase-mediated recombination. Alternatively, if the two recognition sites are located on different molecules, recombinase-mediated recombination will lead to integration of a circular molecule or translocation between two linear molecules. These features make SSRs extremely useful for a number of applications in mammalian systems, including conditional activation of transgenes in mice, chromosome engineering to obtain deletions, translocations or inversions, removal of selection marker genes, gene replacement, targeted insertion of transgenes, and the activation or inactivation of genes by inversion (Nagy, Genesis, 26, 99-109 (2000); Cohen-Tannoudji et al., Mol. Hum. Reprod. 4, 929-938 (1998)).

[0004] In addition to Cre, a few recombinases have been shown to exhibit some activity in mammalian cells. The best characterized examples are the yeast-derived FLP and Kw recombinases, which exhibit optimal activity at 30° C. and are unstable at 37° C. (Buchholz et al., Nature Biotech., 16, 657-662 (1998); Ringrose et al., Eur. J. Biochem., 248, 903-912). Other recombinases that show some activity in mammalian cells include a mutant integrase of phage lamda, the integrases of phage HK022, mutant gamma delta-resolvase and beta-recombinase (Lorbach et al., J. Mol. Biol., 296, 1175-81 (2000); Kolot et al., Mol. Biol. Rep. 26, 207-213 (1999); Schwikardi et al., FEBS Lett., 471, 147-150 (2000); Diaz et al., J. Biol. Chem., 274, 6634-6640 (1999)). The integrase of phage phiC31 (C31-Int) has been found to work in mammalian cells (EP00124629.7; U.S.60/311,876; Groth et al., Proc. Natl. Acad. Science, 97, 5995-6000 (2000)). Moreover, an improved version of the phiC31 integrase has been developed. This modified C31-Int (C31-Int(CNLS)) carries a C-terminal nuclear localization signal (NLS) and displays a recombination efficiency in mammalian cells-that is significantly enhanced over the wild type form and is comparable to that of Cre recombinase (EP00124629.7; U.S.60/311,876). This makes the C31-Int a valuable tool for mammalian genome modification.

[0005] Unlike FLP or Kw, and like the majority of SSRs, the phage derived C31-Int is normally expressed in a prokaryotic organism. Examples of other phage integrase systems include coliphage P4 recombinase, Listeria phage recombinase, bacteriophage R4 Sre recombinase, CisA recombinase, XisF recombinase and transposon Tn4451 TnpX recombinase (Stark et al. Trends in Genetics 8, 432-439 (1992); Hatfull & Gridley, in Genetic Recombination. Eds. Kucherlipati & Smith, Am. Soc. Microbiol., Washington D.C., 357-396 (1988)).

[0006] For use in eukaryotic systems, SSRs should be expressed at high levels. However, expression of prokaryotic genes in eukaryotic systems can face several problems:

[0007] The first problem is codon usage. Through the redundancy of the genetic code, most amino acids are encoded by multiple codons. It has been observed that the codon for a given amino acid is not randomly chosen. Rather, certain codons are preferred, and the frequency of usage of particular codons varies by organism (Ikemura, Mol. Biol Evol. 2, 13-34 (1985); Zhang et al., Gene 105, 61-72 (1991)). The relative frequency of codons is usually correlated to the abundance of the corresponding tRNA (Duret, Trends Genet. 16, 287-289 (2000); Moriyama and Powell, J. Mol. Evol. 45, 514-523 (1997)). For many organisms it has been found that highly expressed genes show a bias in codon usage: they show an over-proportional usage of codons for abundant tRNAs (Grantham et al., Nucleic Acids Res. 9, r43-r74 (1981)). Prokaryotic genes may therefore have a codon composition that is not favorable for high-level expression in eukaryotic systems.

[0008] The second potential problem is splicing. The splicing process is unique to eukaryotic cells and does not occur in prokaryotes. For this reason prokaryotic genes may contain sequence motifs that are recognized as splice donors or splice acceptors when the gene is integrated into the genome of eukaryotic cells. This can lead to aberrant and undesired splicing of the prokaryotic transgene, resulting in a truncated gene product.

[0009] The third potential problem is methylation of the DNA dinucleotide motif CpG in vertebrate cells. Methylcytosine can undergo spontaneous deamination to thymine, resulting in a C to T transition in the DNA sequence. For this reason the CpG dinucleotide is statistically underrepresented in the vertebrate genome. On the other hand, in mammals DNA methylation is often associated with gene silencing (Chomet, Curr. Opin. Cell Biol. 3, 438-443 (1991); Razin, EMBO J. 17, 4905-4908 (1998)). CpG rich prokaryotic genes are therefore prone to gene silencing if introduced into mammalian organisms (Cui et al., Transgenic Res. 3, 182-194 (1994)). Further, unmethylated CpG dinucleotides that are flanked by two 5′ purines and two 3′ pyrimidines (the “immuno-stimulatory CpG motif”) have been shown to stimulate an immune response in vivo and in vitro (Krieg et al., 1995, Nature 374:546-9; Sato et al., Science 273, 352-354 (1996)).

[0010] All these differences between prokaryotic and eukaryotic (mammalian in particular) gene architecture can hamper efficient expression of a phage or bacteria-derived site-specific recombinase in a mammalian organism such as the mouse. For Cre codon-optimized genes with improved expression in mammals have been described (PCT EP01 07729; Koresawa et al., J. Biochem. 127, 367-372 (2000)). However, codon-optimisation has to be performed individually for each new gene, taking into account all factors that can influence gene expression.

SUMMARY

[0011] The present invention provides genetically engineered nucleic acid molecules encoding phiC31-integrase. These nucleic acid molecules, referred to as C31-Int genes, comprise sequences optimized for expression in eukaryotic host cells. In a preferred embodiment, a C31-Int gene comprises at least 306, 430, or 550 codons that are optimal for expression in the host cell. Preferred host cells are from mouse, rat, human, rabbit, and teleost.

[0012] In some embodiments, the optimized C31-Int gene has been further engineered to remove sequences matching consensus 5′ splice donor sequences or consensus 3′ splice acceptor sequences, and/or CpG dinucleotides. The C31-Int gene may contain fewer than 200, 150, 100, or 50 CG dinucleotides, and/or contain few or no immuno-stimulatory CpG motifs with the sequence RRCGYY. A C31-Int gene of the present invention may further comprise a Kozak consensus sequence at the translational start codon, a second termination codon positioned 3′ to the first translational termination codon, and/or a nucleotide sequence encoding a 3′ nuclear localization signal.

[0013] The invention further provides vectors, microorganisms, vertebrate cells, and transgenic organisms comprising optimized C31-Int genes. In some embodiments, a vertebrate cell comprising a C31-Int gene further comprises phiC31 integrase recognition sequences. The invention provides phiC31 integrase proteins encoded by the optimized C31-Int genes, as well as methods of recombining a DNA molecules containing phiC31 integrase recognition sequences, comprising contacting the DNA molecule with a phiC31 integrase encoded by a C31-Int gene of the invention.

BRIEF DESCRIPTION OF THE FIGURES

[0014]FIG. 1 depicts the ROSA26 targeting vector for C31-Int (CNLS) and C31-Int (CNLS)-CO.

[0015]FIG. 2 depicts ROSA26 locus of the C31 reporter mice carrying a C31 substrate reporter construct.

DETAILED DESCRIPTION

[0016] The invention provides nucleic acid sequences encoding the recombinase phiC31-Integrase (“C31-Int”), where the nucleic acid sequences have been genetically engineered for expression in a eukaryotic host. The term “native (or wild-type) C31-Int gene” refers to a gene that is naturally occurring and/or has not been modified through human intervention, as presented in SEQ ID NO:1. The protein sequence encoded by the native C31-Int is provided in SEQ ID NO:2. The changes introduced into the coding sequence are typically “silent mutations,” meaning that they do not result in changes to the amino acid sequence. As used herein, the term “C31-Int gene” refers to the nucleic acid molecule encoding a C31-Int protein. The C31-Int gene typically includes a translational initiation codon, as well as a translational termination codon. Gene regulatory sequences, including upstream enhancers and/or promoters and a downstream polyadenylation signal, all of which may be heterologous, are usually operably linked to the C31-Int gene. The coding sequence may also comprise heterologous, in-frame coding sequences fused to the recombinase coding sequence. As used herein, the term “optimized C31-Int gene” refers to a C31-Int gene that has been genetically engineered to comprise at least one of the modifications disclosed herein. The invention further provides methods of optimizing the C31-Int coding sequence.

[0017] The present invention is described using the following conventions for describing nucleic acid sequences. Sequences are presented in the 5′ to 3′ direction. Nucleotides may be referred to by the bases they comprise. “A” represents a nucleotide comprising the purine base adenine; “G” represents a nucleotide comprising the purine base guanine; “C” represents a nucleotide comprising the pyrimidine base cytosine, and “T” represents a nucleotide comprising the pyrimidine base thymine. Thus when it is said that, for instance, the fourth and fifth position of a nucleotide sequence consist of a G and a T, it is meant that these positions in the corresponding nucleic acid molecule consist of a nucleotide comprising a guanine base and a nucleotide comprising a thymine base, respectively. “Y” represents either a T or a C; “R” represents either an A or a G, and “N” represents any base (A, C, G, or T). With respect to sequences that represent splice junctions, capital letters represent exon sequence, and lower case letters represent intron sequence. Letters that are within brackets represent the alternative bases that can occur at the given position; percentage values may be included within brackets to indicate the frequencies at which particular bases occur. Intron and exon sequences are depicted in lower and upper case letters for convenience only. It will be understood that with respect to a nucleic acid molecule, there is no structural difference between nucleotides designated as intron or exon sequence. Moreover, in terms of the phiC31 gene sequences of the present invention, all bases will be coding sequence (i.e., “exon”) with respect to the integrase (i.e., even when they are may be recognized as splice junctions and are therefore depicted using include some lower case letters).

[0018] In a preferred embodiment, the C31 nucleic acid sequence is “codon optimized.” To optimize the C31-Int gene sequence for expression in eukaryotic species, silent mutations are introduced into the coding sequence to change the codon encoding a given amino acid to the codon that is most frequently used in the respective host. Such codon usage data is available for a large number of eukaryotic organisms, and, as sequencing of eukaryotic genomes and expressed sequences progresses, is continually being generated (see for instance, the website at www.kazusa.or.jp/codon/). Table 1 contains data for mouse (Mus musculus), rat (Rattus norvegicus), rabbit (Oryctolagus cuniculus), human (Homo sapiens), and zebrafish (Danio rerio). Frequencies of codon usage per thousand are shown for each triplet. The data source was the codon usage database (website at www.kazusa.or.jp/codon/). TABLE 1 Codon frequencies for bacteriophage phiC31, mouse, rat, rabbit, zebrafish, and human. frequency per thousand frequency per thousand mus rattus oryctolagus homo denio mus rattus oryctolagus homo denio triplet phiC31 musculus norvegicus cuniculus sapiens rerio triplet phiC31 musculus norvegious cuniculus sapiens rerio UUU 2.7 16.0 16.3 16.7 17.0 16.9 CUU 24.3 12.3 12.0 10.0 12.8 11.6 UUC 27.4 21.6 24.2 29.0 20.5 21.8 CUC 14.9 19.6 20.7 23.4 19.3 16.8 UUA 0.0 6.0 5.4 5.2 7.3 6.1 CUA 2.2 7.5 7.2 4.9 7.0 5.7 UUG 6.1 12.5 12.2 10.8 12.5 11.6 CUG 27.2 39.3 41.5 48.2 39.7 35.3 UCU 3.7 15.4 14.4 10.4 14.8 16.8 CCU 5.2 18.7 17.1 12.8 17.3 16.7 UCC 12.5 18.1 18.2 19.4 17.5 18.4 CCC 1.2 19.1 18.4 20.7 20.0 15.5 UCA 2.6 11.2 10.6 7.7 11.9 13.2 CCA 1.0 17.3 15.7 11.9 16.7 16.1 UCG 19.4 4.5 4.4 5.4 4.5 7.2 CCG 32.4 6.8 6.5 8.3 7.0 10.6 UAU 5.7 11.8 11.5 9.9 12.1 12.8 CAU 2.8 9.9 9.1 7.4 10.5 10.5 UAC 21.5 16.8 17.7 19.9 15.8 19.5 CAC 15.0 15.3 14.8 16.3 14.9 17.4 UAA 0.7 0.6 0.6 0.5 0.7 0.8 CAA 3.1 11.6 10.6 9.1 12.0 11.7 UAG 0.8 0.5 0.5 0.5 0.5 0.4 CAG 20.4 34.5 33.0 32.6 34.5 33.5 UGU 2.4 10.9 9.6 8.2 10.0 11.1 CCU 12.8 4.7 4.9 3.8 4.6 6.9 UGC 8.2 12.6 12.1 13.2 12.3 13.6 CGC 29.2 10.1 10.2 13.1 10.8 10.5 UGA 2.7 1.1 1.0 1.0 1.3 1.1 CGA 5.0 6.7 6.6 5.1 6.3 6.9 UGG 19.3 12.9 13.2 14.0 12.9 11.8 CGG 21.3 10.5 10.7 11.5 11.6 7.5 AUU 14.1 14.6 15.4 14.5 15.8 15.9 GUU 17.6 10.1 10.0 9.0 10.9 12.1 AUC 19.5 22.9 26.1 30.2 21.6 24.2 GUC 29.9 15.6 16.9 18.1 14.6 14.5 AUA 0.9 6.6 6.6 6.0 7.2 6.8 GUA 3.8 6.9 7.0 4.9 7.0 6.1 AUG 18.6 22.2 23.7 24.4 22.3 27.0 GUG 29.4 29.0 30.7 33.3 28.8 26.5 ACU 8.0 13.2 12.8 10.1 12.9 13.6 GCU 18.7 19.7 19.5 15.7 18.5 19.3 ACC 18.5 19.6 20.6 22.1 19.3 18.7 GCC 49.2 26.7 28.1 33.9 28.3 20.9 ACA 2.0 15.6 15.1 11.6 14.9 15.6 GCA 9.5 15.5 15.2 12.8 15.9 15.5 ACG 39.5 6.1 6.4 8.9 6.3 8.4 GCG 45.6 7.1 6.9 8.8 7.5 9.7 AAU 3.5 15.5 15.0 13.3 17.0 15.7 GUN 6.6 21.4 20.7 17.9 22.4 21.3 AAC 24.7 21.5 22.6 24.2 19.8 26.8 GAC 63.1 27.5 28.5 30.9 26.1 28.8 AAA 1.3 21.3 20.5 20.3 24.0 25.2 GAA 26.7 26.9 25.9 24.7 29.1 21.1 AAG 45.5 34.6 35.3 35.2 32.6 28.6 GAG 34.9 40.3 40.8 43.7 40.2 38.8 AGU 3.5 12.2 11.4 8.5 12.0 13.0 GGU 17.1 11.7 11.2 9.0 10.8 14.0 AGC 11.6 20.0 19.3 19.1 19.3 21.6 GGU 44.5 22.9 22.6 26.5 22.7 19.1 AGA 0.7 11.4 10.4 9.2 11.5 12.7 GGA 7.0 17.3 16.4 14.9 16.4 21.1 AGG 1.3 11.6 11.4 10.4 11.3 10.3 GGG 17.5 15.9 15.8 17.0 16.4 10.2

[0019] As used herein, the terms “codon that is optimal for expression in the eukaryotic host cell” and “optimal host codon” refer to the codon sequence that is most utilized by the particular host. If two codon sequences are essentially equally utilized (e.g., within approximately 1-2%), the optimal codon can refer to either of these sequences. Table 1 (as well as Table 4, below) further provides the second, third, fourth, fifth and sixth most prevalent codon sequences for the particular species. It will be understood that different amino acids are encoded 1, 2, 3, 4, or 6 codons (e.g., Met is encoded by one codon, Cys by two, and Ser by six). Thus, general reference to a second, third, fourth, etc. most prevalent codon refers to as many codons exist for any particular amino acid. For a sequence optimized for a particular host, preferably at least 50%, more preferably at least 70%, and most preferably at least 90% of the codons in the codon-optimized gene will be identical to an optimal host codon. The nucleotide sequence encoding C31-Int preferably comprises at least 306, more preferably at least 430, and more preferably at least 550 codons that are optimal for expression in the particular host.

[0020] The sequence may be further engineered to eliminate potential splice sites that can lead to aberrant splicing after integration into the host genome. The codon-optimized sequence is analyzed for motifs matching either the splice donor or the splice acceptor consensus sequences. The nine nucleotide consensus for the 5′ splice donor site is characterized by the sequence [A,C]Aggt[a,g]agt (Zhuang and Weiner, Cell 46, 827-835 (1986); Stamm et al., DNA and Cell Biology, 19, 739-756 (2000)). Only the GT dinucleotide at the exon/intron boundary (i.e., the G and T in, respectively, the fourth and fifth positions of the consensus) is 100% conserved. At the other positions, alternative nucleotide usage is found with certain frequencies. The consensus sequence is therefore more appropriately described by [C40%, A30%, G20%, C10%] [A70%, G10%, C10%, T10%] [G70%, A15%, T10%, C5%] [g100%] [t100%] [a60%, g30%, c5%, t5%] [a55%, t15%, c12.5%, g12.5%] [g70%, a12.5%, t10%, c7.5%] [t50%, a20%, g20%, c10%]. Sequences matching variations of the consensus may also be changed to sequences less favorable for splicing through silent mutations. Such silent mutations most preferably replace the optimal codon with the second most prevalent codon and may also replace the optimal codon with the third or fourth most prevalent codon.

[0021] In one embodiment, the nucleic acid molecule of the present invention does not contain a splice donor sequence, wherein the splice donor sequence is AAGgtaagt, AAGgtgagt, CAGgtaagt, or CAGgtgagt. In other embodiments, the nucleic acid molecule of the present invention does not contain a splice donor sequence comprising nine contiguous nucleotides, wherein the fourth and fifth are, respectively, G and T, and wherein at least three, four, or five of the nucleotides in the first, second, third, six, seventh, eighth, and/or ninth positions are identical to the nucleotide in the corresponding position in the sequence AAGgtaagt, AAGgtgagt, CAGgtaagt, or CAGgtgagt. In each case, the “corresponding nucleotide” is determined simply by counting, starting with “1” for the first nucleotide of a 9-nucleotide sequence. As illustration, a nucleic acid molecule that comprises the sequence “CTCGTCATT” would be said to contain a splice donor sequence where the fourth and fifth positions are G and T, respectively, and three additional bases—those in the first, seventh, and ninth positions—are identical to the nucleotide in the corresponding position of CAGgtaagt.

[0022] The nucleic acid of the present invention may alternatively or additionally be engineered to eliminate potential 3′ splice acceptor sequences. The 3′ splice acceptor site is characterized by the twelve base consensus sequence yyyyyyyncagG (Moore, Nature Struct. Biol. 7, 14-16 (2000); Stamm et al., DNA and Cell Biology, 19, 739-756 (2000)). However, only the AG dinucleotide at the intron/exon boundary (i.e., the A and G in, respectively, the tenth and eleventh positions of the consensus) is 100% conserved. At the other positions, alternative nucleotide usage is found with certain frequencies. The consensus sequence is therefore more appropriately described by yyyyyyyn [c80%, t20%] [a100%] [g100%] [G50%, A20%, C20%, T10%] (Stamm et al., DNA and Cell Biology, 19:739-756, 2000). Sequences matching any of these variations of the consensus sequence may be changed to sequences less favorable for splicing through silent mutations. Such silent mutations most preferably replace the optimal codon with the second most prevalent codon and may also replace the optimal codon with the third or fourth most prevalent codon.

[0023] In one embodiment, the nucleic acid molecule of the present invention does not contain a splice acceptor sequence, wherein the splice acceptor sequence is yyyyyyyncagG (SEQ ID NO:3) or yyyyyyyntagG (SEQ ID NO:4). It will be understood that since each “Y” can represent either C or T, and “N” can represent any base, each sequence of SEQ ID NO:3 and each sequence of SEQ ID NO:4 actually represents 512 (2⁷×4) distinct sequences. In other embodiments, the nucleic acid molecule of the present invention does not contain a splice acceptor sequence comprising twelve contiguous bases, wherein the ninth position is a C or T, wherein the tenth and eleventh bases are, respectively, A and G, and wherein at least four or five of the bases in the first, second, third, fourth, fifth sixth, seventh, and twelfth positions are identical to the base in the corresponding position in any of the sequences of SEQ ID NO:3 or 4. For illustration, a nucleic acid molecule that comprises the sequence “CTACAAGGTAGG” would be said to contain a splice acceptor sequence where the tenth and eleventh positions are, respectively, A and G, the ninth position is T, and four additional bases—those in the first, second, fourth and twelfth positions—are identical to a base in the corresponding position of CTYCYYYNTAGG, which is one of the sequences represented by SEQ ID NO:4 (yyyyyyyntagG).

[0024] The nucleic acid molecule of the present invention may be further engineered to reduce the number of CG (“CpG”) dinucleotides, in order to minimize the risk of inactivation of the C31-Int transgene through methylation by DNA-cytosine-5-methyltransferase at CpG dinucleotides (Pfeifer et al., EMBO J. 4:2879-2884, 1985). In general, the number of CpG dinucleotides is reduced as much as possible while still maintaining a preferred codon composition (e.g, at least 50% of C31-Int codons are optimal for the eukaryotic host). Reduction of CpG dinucleotides generally occurs through introduction of silent mutations, which most preferably replace the optimal codon with the second most prevalent codon, and may also replace the optimal codon with the third or fourth most prevalent codon. For an optimized C31-Int gene sequence, the number of CpG dinucleotides is preferably reduced by at least 40%, more preferably by at least 70% and most preferably by at least 90-100%. In preferred embodiments, the codon optimized C31-Int nucleic acid molecule comprises fewer than 200, 150, 100, or 50 CpG dinucleotides, or comprises no CpG dinucleotides. The codon optimized C31-Int may also be engineered to specifically eliminate “immuno-stimulatory” CpG motifs, which comprise the sequence RRCGYY. In one embodiment, the C31-Int nucleic acid molecule of the present invention does not comprise the sequence RRCGYY. In a further embodiment, a C31-Int gene that has been codon optimized, and has been engineered to reduce potential splice sites and CpG motifs, has the sequence presented in SEQ ID NO:5.

[0025] Other modifications may be made to further engineer the C31-Int gene for optimal expression of the C31-Int protein. In one embodiment, the C31-Int gene is engineered with a Kozak consensus sequence that spans the translational start codon. Kozak consensus sequences are generally represented by the sequence: GCCRCCATGG, in which the “ATG” represents the translational start codon, and may differ according to species (see, e.g., Kozak M, Cell 44:283-92, 1986; Kozak M, Nucleic Acids Res 15:8125-48, 1987; Kozak M, J Cell Biol 108:229-241, 1989; Jacobs G H et al., Nucleic Acids Res 30:310-1, 2002).

[0026] In another embodiment, the C31-Int gene also comprises sequence encoding a nuclear localization signal (NLS) to facilitate the import of cytoplasmic proteins into the nucleus (see, e.g., Gorlich et al., Science 271:1513-1518, 1996). Numerous NLS sequences, which share a high proportion of basic amino acids, have been characterized (see, e.g., Boulikas, Crit. Rev. Eucar. Gene Expression 3:193-227, 1993); a prototypical NLS of seven amino acids is derived from the T-antigen of the SV40 virus (Kalderon et. al, Cell, 39, 499-509 (1984)). Exemplary C31-Int genes comprising C-terminal NLS sequences are provided in SEQ ID NO:8 and SEQ ID NO:13, as further described in the Examples.

[0027] In yet another embodiment, the C31-Int gene is engineered with a second translational termination codon positioned 3′ to the first translational termination codon, preferably immediately 3′ thereto, and 5′ to the polyadenylation signal. This second stop codon is added to ensure proper translational termination.

[0028] A nucleic acid of the present invention encodes a C31-Int that is functionally active and is capable of catalyzing recombination at C31-Int recognition sequences in a eukaryotic host cell. As used herein, a C31-Int “that catalyzes recombination at phiC31 recognition sequences in the eukaryotic host cell” is one that is capable of catalyzing recombination at the recognition sequences. C31-Int recognition sequences, designated “attP” and “attB” are known in the art (Thorpe et al. Proc. Natl. Acad. Sci. USA, 95, 5505-5510 (1998)). Minimal recognition sequences have also been described (Groth et al., Proc. Natl. Acad. Science, 97, 5995-6000 (2000)). A functionally active C31-Int may catalyze recombination at any site known to be recognized by the native C31-Int.

[0029] A functionally active C31-Int generally has the protein sequence presented in SEQ ID NO:2. However, one or more changes in the amino acid sequence may be made without eliminating recombinase activity. Such changes are usually conservative. A conservative amino acid substitution is one in which an amino acid is substituted for another amino acid having similar properties such that the folding or activity of the protein is not significantly affected. Aromatic amino acids that can be substituted for each other are phenylalanine, tryptophan, and tyrosine; interchangeable hydrophobic amino acids are leucine, isoleucine, methionine, and valine; interchangeable polar amino acids are glutamine and asparagine; interchangeable basic amino acids are arginine, lysine and histidine; interchangeable acidic amino acids are aspartic acid and glutamic acid; and interchangeable small amino acids are alanine, serine, threonine, cysteine and glycine.

[0030] A variety of systems for determining whether a codon optimized C31-Int retains functional recombinase activity are known in the art and include systems for directly assessing the nucleic molecules that were recombined, as well as indirectly assessing recombinase activity through, for instance, a reporter gene which is activated, inactivated, or eliminated as a result of recombination. Such experiments may use cell-free systems comprising all the necessary components for recombination, or may use cultured cells or transgenic animals that have been engineered to express the C31-Int. Exemplary systems are further described in the Examples 2 and 3. A functionally active C31-Int preferably catalyzes recombination at least as efficiently as the wild type C31-Int, and more preferably catalyzes recombination at a higher level than the wild-type C31-Int.

[0031] Furthermore, a functionally active C31-Int encoded by an optimized C31-Int gene is preferably expressed at levels that are at least comparable to and more preferably higher than those encoded by a native C31-Int gene. The term “expression” refers to both transcription (mRNA levels) and translation (protein levels). Thus, in one embodiment it is preferred that in a given host, a codon-optimized C31-Int gene is transcribed at a comparable or higher level than a wild-type C31-Int gene, assuming that transcription of both is directed by essentially the same regulatory sequences. In another embodiment it is preferred that in a given host, protein expression from a codon optimized C31-Int gene is comparable to or higher than that from a wild-type C31-Int gene, assuming that the corresponding mRNAs are expressed at essentially comparable levels. Methods for analyzing mRNA and protein expression are well known in the art. For instance, Northern blotting, slot blotting, ribonuclease protection, or quantitative RT-PCR (e.g., using the TaqMan®, PE Applied Biosystems) may be used to assess mRNA expression (e.g., Current Protocols in Molecular Biology (1994) Ausubel F M et al., eds., John Wiley & Sons, Inc., chapter 4; Freeman W M et al., Biotechniques (1999) 26:112-125). Protein expression may be monitored with specific antibodies or antisera directed against either the C31-Int protein or specific peptides. A variety of means, including Western blotting, ELISA, or in situ detection, are available (Harlow E and Lane D, 1988, Antibodies: A Laboratory Manual, CSH Laboratory Press, New York).

[0032] An engineered C31-Int gene may differ in its methylation status (i.e., the proportion of methylated CpG dinucleotides) from a native C31-Int gene. Thus, further assessment of an engineered C31-Int gene may include detection of its methylation status, which is typically performed by Southern analysis and shows certain enzymes' inability to digest methylated DNA.

[0033] The present invention is directed to nucleic acid molecules comprising optimized C31-Int genes. Codon optimized C31-Int nucleic acid molecules may be generated by any available means. In one example, the generation of the synthetic gene involves annealing oligonucleotides to generate small subfragments, ligation of these subfragments to generate larger fragments, and eventual ligation of the full-length gene fragment (Scrable and Stambrook, Genetics 147, 297-304 (1997); EP1005574). As used herein, the term “genetic engineering” refers to any method of generating a nucleic acid molecule that differs from the corresponding native nucleic acid molecule. Accordingly, a genetically engineered nucleic acid molecule encoding a C31-Int is one that has been produced through human manipulation. A C31-Int gene may be inserted in a cloning vector, including bacteriophages such as lambda derivatives, or plasmids such as PBR322, pUC plasmid derivatives and the Bluescript vector (Stratagene, San Diego, Calif.). A C31-Int gene can be inserted into any appropriate expression vector for the transcription and translation of the inserted protein-coding sequence. Exemplary expression vectors are further described in the Examples. A variety of host-vector systems may be utilized to express the protein-coding sequence such as mammalian cell systems infected with virus (e.g. vaccinia virus, adenovirus, etc.); insect cell systems infected with virus (e.g. baculovirus); microorganisms such as yeast containing yeast vectors, or bacteria transformed with bacteriophage, plasmid or cosmid DNA. The present invention encompasses vectors comprising an optimized C31-Int gene, as well as microorganisms transformed with such vectors. A preferred microorganism is E. coli.

[0034] The present invention is further directed to cultured eukaryotic cells and non-human transgenic organisms that harbor a nucleic acid molecule comprising an optimized C31-Int gene in their genomes. Non-native nucleic acid is introduced into cultured cells or non-human laboratory animals by any expedient method. Preferred cultured cells are vertebrate cells, particularly those derived from mouse, rat, human, rabbit, or zebrafish. Methods for generating transformed cells are known in the art and include transfection, electroporation, particle bombardment, viral or retroviral infection, etc. Preferred transgenic animals are mammals, particularly mice or rats, and teleost, such as zebrafish. Methods of making transgenic non-human organisms are well-known in the art (see, e.g., for mice: Brinster et al., Proc. Nat. Acad. Sci. USA 1985, 82:4438-42; U.S. Pat. Nos. 4,736,866, 4,870,009, 4,873,191, 6,127,598; Hogan, B., Manipulating the Mouse Embryo, Cold Spring Harbor Laboratory Press, Cold Spring Harbor, N.Y., 1986; for rats: Murphy, D. and Carter, D. A. (1993) Transgenesis Techniques, Principles and Protocols, Humana, Totowa, N.J.; Mullins L J and Mullins J J, J Clin Invest 97:1557-60, 1996; for zebrafish: Lin S, Methods Mol Biol 136:375-383, 2000; Linney et al., Dev Biol 213:207-16, 1999; Ju et al., Dev Genet 25:158-67, 1999).

[0035] Cultured cells and transgenic animals of this invention, which comprise an optimized C31-Int gene in their genome, may further comprise C31-Int recognition sequences, also known as “att” sequences. Typically, for the production of doubly transgenic animals, two transgenic animal strains are generated, one comprising the recombinase gene and the other comprising recognition sequences, and the two components are brought into the same animal by crossing. Methods for using recombinase systems (i.e., a recombinase and associated recognition sites) for studying gene function are well known in the art (see, e.g., Rajewsky et al., J. Clin. Invest., 98,:600-603, 1996; Nagy, Genesis, 26:99-109,2000). The system comprising the C31-Int gene and its recognition sequences provides for the controlled activation or inactivation of genes of interest, and accordingly, methods for studying the function of such genes. When the recognition sites flank a particular gene of interest, expression of the recombinase can effect elimination (knock-out) of that gene in host cells. If the recognition sites are placed in inverted orientation, the flanked DNA sequence can be inverted. Alternatively, if the recognition sequences flank a sequence that interrupts a gene of interest, expression of the recombinase can effect activation of that gene by eliminating the disrupting sequence. Furthermore, the att-flanked DNA sequence can be exchanged for a different att-flanked sequence that is co-introduced with the C31-Int. In certain embodiments, the recombinase is expressed under the control of tissue- or temporal-specific promoters, such that the gene of interest is specifically activated or inactivated at particular developmental time points or only in particular tissues. The recombinase may also be expressed under the control of regulatory elements that are specifically activated in response to external agents, such as a hormone, an antibiotic (e.g., tetracycline), etc.

[0036] All references cited herein, including patents, patent applications, and publications, are herein incorporated by reference in their entireties.

EXAMPLES Example 1 Design of a C31-Int Gene for Expression in Mouse Cells

[0037] A version of a C31-Int gene that had been previously engineered to include sequence encoding a nuclear localization signal, designated C31-Int (CNLS), was further engineered for expression in mouse cells. The original nucleic acid sequence encoding C31-Int (CNLS) is presented in SEQ ID NO:6, and the corresponding protein sequence is presented in SEQ ID NO:7.

[0038] To design a C31-Int (CNLS) gene sequence with optimal properties for expression in the mouse, silent mutations were introduced into the wild type coding sequence (SEQ ID NO:6), and codons for particular amino acids were changed to the optimal codons for those amino acids in the mouse, as presented in Tables 1 and 4 (below).

[0039] In the next step, this codon-optimized sequence was analyzed for motifs matching either the splice donor or the splice acceptor consensus sequences. Sequences matching the 5′ splice donor consensus were found at four positions in the codon-optimized C31-Int gene. To eliminate these potential splice sites, these four sequences were changed to sequences less favorable for splicing through silent mutations in which the optimal codon was replaced with the second most prevalent codon (see Tables 1 and 4). Sequences matching the 3′ splice acceptor consensus were found at two positions in the gene and were changed to sequences less favorable for splicing through silent mutations replacing the optimal codon with the second or third most prevalent codon. Table 2 shows the silent mutations introduced to eliminate potential splice sites from the codon-optimized C31-Int(CNLS) gene. The “consensus sequences,” as shown for the 5′ splice donor and the 3′ splice acceptor sites, refer to motifs that were present in an “intermediate sequence” derived following codon-optimization of the C31-Int(CNLS) gene (and may therefore not be present in the C31-Int(CNLS) nucleotide sequence presented in SEQ ID NO:6). The “modified sequences” have incorporated the silent mutations and are present in the optimized C31-Int gene presented in SEQ ID NO:8. Numbering of nucleotides refers to the position within the C31-Int(CNLS) gene, the A of the ATG start codon being +1. Nucleotides that were altered are underlined. Capital letters refer to exon sequence, and lower case letters refer to intron sequence. Sequences are shown with nucleotides grouped according to codons. TABLE 2 Silent mutations introduced to eliminate potential splice sites. Elimination of 5′ splice donor consensus Elimination of 3′ splice acceptor consensus Position of 5′ Consensus Modified Position of 3′ Consensus Modified consensus sequence sequence consensus sequence sequence 316-324 AAG gtg atg AAG gtc atg  94-105 gcc acc cag agG c gcc acc cag agA 337-345 ATC gtg agc ATC gtg tcc 868-879 agg gac ccc agG g agg gac ccc cgG 553-561 CTG gtg agc CTC gtg agc 1179-1187 C AGg tgc ag C AGa tgc ag

[0040] Through this codon-optimization process, the number of CpG methylation sites was simultaneously reduced. To further reduce the number of CpG dinucleotides and in parallel eliminate immuno-stimulatory CpG motifs from the gene sequence, the CpG dinucleotide motif was altered at 20 positions matching the consensus for immuno-stimulatory CpGs (RRCGYY), as shown in Table 3. To eliminate the CpG dinucleotide, individual codons were replaced by the second most prevalent codon for the particular amino acid. Table 3 shows the silent mutations introduced to eliminate potential immuno-stimulatory CpG motifs. As in Table 2, the “consensus sequences,” refer to motifs that were present in an “intermediate sequence” derived following codon-optimization of the C31-Int(CNLS) gene, and the “modified sequences” are present in the optimized C31-Int gene presented in SEQ ID NO:8. Numbering of nucleotides refers to the position within the C31-Int(CNLS) gene, the A of the ATG start codon being +1. Nucleotides that were altered are underlined. Sequences are shown with nucleotides grouped according to codons. TABLE 3 Silent mutations introduced to eliminate CpG motifs. Position of RRCGYY Consensus Modified consensus sequence sequence 40-45 ggc gcc gga gcc 79-84 agc gcc tcc gcc 106-111 agc gcc tcc gcc 205-210 agc gcc tcc gcc 235-330 gac gcc gat gcc 442-447 gac gcc gat gcc 472-477 agc gcc tcc gcc 778-783 gac gcc gat gcc 784-789 gac gcc gat gcc 832-837 agc gcc tcc gcc 1099-1104 agc gcc tcc gcc 1129-1134 ggc gcc gga gcc 1210-1215 agc gcc tcc gcc 1420-1425 gac gcc gat gcc 1429-1434 aac gcc aat gcc 1465-1470 ggc gcc gga gcc 1537-1542 ggc gcc gga gcc 1612-1617 gac gcc gat gcc 1618-1623 gac gcc gat gcc 1807-1812 gac gcc gat gcc

[0041] Overall, the number of CpG dinucleotides was reduced from 245 in the wild type C31-Int(CNLS) gene (SEQ ID NO:6) to 132 in the codon-optimized gene (SEQ ID NO:8).

[0042] To further improve expression, the sequence GCCACC was attached 5′ to the ATG start codon in order to generate a close match to the Kozak consensus sequence GCCRCCATGG. A second stop codon (TGA) was added at the 3′ terminus of the coding sequence to ensure proper translational termination.

[0043] Finally, the gene was flanked by restriction enzyme (EcoRV) sites for cloning purposes. The sequence nucleotide sequence of the optimized C31-Int gene, designated C31-Int(CNLS)-CO, is provided in SEQ ID NO:8.

[0044] The engineered gene was synthesized by GeneArt (Regensburg, Germany).

[0045] Table 4 shows the codon usage for each amino acid in the wild type version of C31-Int(CNLS) and C31-Int(CNLS)-CO, as well as codon usage in phiC31 and in mouse. Number of occurrences (#) and frequencies per thousand(/1000) are displayed. TABLE 4 Codon frequencies in C31-Int(CNLS) and C31-Int(CNLS)-CO phiC31 mus C31-Int(CNLS)- Amino phage/ musculus/ C31-Int(CNLS) CO acid triplet 1000 1000 # /1000 # /1000 ARG CGA 5 6.7 3 4.8 0 0.0 CGC 29.2 10.1 25 40.3 0 0.0 CGG 21.3 10.5 14 22.5 1 1.6 CGU 12.8 4.7 5 8.1 0 0.0 AGA 0.7 11.4 0 0.0 3 4.8 AGG 1.3 11.6 6 9.7 49 78.9 Leu CUA 2.2 7.5 0 0.0 0 0.0 CUC 14.9 19.6 9 14.5 1 1.6 CUG 27.2 39.3 12 19.3 42 67.6 CUU 24.3 12.3 18 29.0 0 0.0 UUA 0 6 0 0.0 0 0.0 UUG 6.1 12.5 4 6.4 0 0.0 SER UCA 2.6 11.2 2 3.2 0 0.0 UCC 12.5 18.1 4 6.4 8 12.9 UCG 19.4 4.5 16 25.8 0 0.0 UGU 3.7 15.4 2 3.2 0 0.0 AGC 11.6 20 8 12.9 25 40.3 AGU 3.5 12.2 1 1.6 0 0.0 THR ACA 2 15.6 2 3.2 0 0.0 ACC 18.5 19.6 9 14.5 37 59.6 ACG 39.5 6.1 21 33.8 0 0.0 ACU 8 13.2 5 8.1 0 0.0 PRO CCA 1 17.3 1 1.6 0 0.0 CCC 1.2 19.1 9 14.5 33 53.1 CCG 32.4 6.8 18 29.0 0 0.0 CCU 5.2 18.7 5 8.1 0 0.0 ALA GCA 9.5 15.5 7 11.3 0 0.0 GCC 49.2 26.7 24 38.6 65 104.7 GCG 45.6 7.1 27 43.5 0 0.0 GCU 18.7 19.7 7 11.3 0 0.0 GLY GGA 7 17.3 5 8.1 4 6.4 GGC 44.5 22.9 25 40.3 47 75.7 GGG 17.5 15.9 19 30.6 0 0.0 GGU 17.1 11.7 2 3.2 0 0.0 VAL GUA 3.8 6.9 4 6.4 0 0.0 GUC 29.9 15.6 17 27.4 1 1.6 GUG 29.4 29 8 12.9 37 59.6 GUU 17.6 10.1 9 14.5 0 0.0 LYS AAA 1.3 21.3 2 3.2 1 1.6 AAG 45.5 34.6 39 62.8 40 64.4 ASN AAC 24.7 21.5 11 17.7 12 19.3 AAU 3.5 15.5 2 3.2 1 1.6 GLN CAA 3.1 11.6 6 9.7 0 0.0 CAG 20.4 34.5 13 20.9 19 30.6 HIS CAC 15 15.3 9 14.5 10 16.1 CAU 2.8 9.9 1 1.6 0 0.0 GLU GAA 26.7 26.9 26 41.9 1 1.6 GAG 34.9 40.3 26 41.9 51 82.1 ASP GAC 63.1 27.5 40 64.4 32 51.5 GAU 6.6 21.4 1 1.6 9 14.5 TYR UAC 21.5 16.8 10 16.1 12 19.3 UAU 5.7 11.8 2 3.2 0 0.0 CYS UGC 8.2 12.6 5 8.1 7 11.3 UGU 2.4 10.9 2 3.2 0 0.0 PHE UUC 27.4 21.6 19 30.6 19 30.6 UUU 2.7 16 0 0.0 0 0.0 ILE AUA 0.9 6.6 0 0.0 0 0.0 AUC 19.5 22.9 18 29.0 31 49.9 AUU 14.1 14.6 13 20.9 0 0.0 MET AUG 18.6 22.2 11 17.7 11 17.7 TRP UGG 19.3 12.9 11 17.7 11 17.7 TER UAA 0.7 0.6 0 0.0 0 0.0 UAG 0.8 0.5 1 1.6 0 0.0 UGA 2.7 1.1 0 0.0 1 1.6

[0046] A second codon optimized C31-Int gene, designated “C31-Int(CNLS)-CO-delCG,” was designed and generated (synthesized by GeneArt [Regensburg, Germany]); its sequence is presented in SEQ ID NO:13. Like the C31-Int(CNLS)-CO (SEQ ID NO:8), it comprises a Kozak consensus sequence, a second stop codon, and sequence encoding a carboxy-terminal NLS. However, C31-Int(CNLS)-CO-delCG was specifically engineered to eliminate all CG dinucleotides from its coding sequence.

Example 2 Functional Analysis of C31-Int(CNLS)-CO

[0047] In order to test the activity of the codon-optimized form of C31-Int(CNLS) (“C31-Int(CNLS)-CO”) in mouse cells, the activities of expression vectors comprising C31-Int(CNLS) and C31-Int(CNLS)-CO genes were compared.

[0048] A. Description of Plasmids

[0049] The C31-Int(CNLS) expression vector, whose sequence is presented in SEQ ID NO:9, was designated pCMV-C31-Int(CNLS) and was generated using the C31-Int gene sequence amplified from phage DNA (DSM-49156, DSMZ-Deutsche Sammlung von Mikroorganismen und Zellkulturen GmbH, Mascheroder Weg 1b, D-38124 Braunschweig, Germany). The stop codon of the native C31-Int sequence was replaced by a 21 bp sequence encoding the 7 amino acid SV40 T-antigen NLS (PKKKRKV; Kalderon et al., 1984), followed by a new stop codon. pCMV-C31-Int(CNLS) comprises the following sequence: a 700 bp cytomegalovirus immediate early gene promoter (position 12-711), a 270 bp hybrid intron (position 712-981), the NLS-modified C31-Int gene (position 989-2851), and a 189 bp synthetic polyadenylation sequence (position 2854-3043).

[0050] The C31-Int(CNLS)-CO expression vector, whose sequence is presented in SEQ ID NO: 10, was designated pCMV-C31-Int(CNLS)-CO and is similar to pCMV-C31-Int(CNLS), except that it comprises C31-Int(CNLS)-CO instead of C31-Int(CNLS).

[0051] Activities of the expression vectors pCMV-C31-Int(CNLS) and pCMV-C31-Int(CNLS)-CO were tested in reporter cells that contained a stably integrated “substrate vector,” comprising a beta-galactosidase coding sequence under control of an upstream SV40 promoter. The coding sequence was separated from the promoter and functionally disrupted by insertion of a 1.1 kb puromycin gene cassette (containing a stop codon and a polyadenylation sequence), and the cassette was flanked by C31-Int recognition sequences (5′, the 84 bp attB, and 3′, the 84 bp attP) adjacent to direct repeat loxP sites. Upon either C31-Int- or Cre-mediated recombination, the termination cassette would be deleted, allowing expression of beta-galactosidase.

[0052] The substrate vector, whose sequence is presented in SEQ ID NO: 11, was designated “pRK64” and was generated using the PSV-Pax1 vector backbone (Buchholz et al., Nucleic Acids Res. 24:4256-4262,1996).

[0053] All vectors were generated using standard molecular biology and recombinant DNA cloning techniques and their nucleotide sequences confirmed by DNA sequence analysis.

[0054] B. Cell Culture and Transfections:

[0055] To generate a stably transfected reporter cell line, 2.5×10⁶ NIH-3T3 cells (Andersson et al., Cell, 16, 63-75 (1979); DSMZ#ACC59; DSMZ-Deutsche Sammlung von Mikroorganismen und Zellkulturen GmbH, Mascheroder Weg 1b, D-38124 Braunschweig, Germany) were electroporated with 5 μg pRK64 plasmid DNA linearized with ScaI and plated into 10 cm petri dishes. The cells were grown in DMEM/Glutamax medium (Life Technologies) supplemented with 10% fetal calf serum at 37° C., 10% CO₂ in humid atmosphere, and passaged upon trypsinization. Two days after transfection the medium was supplemented with 1 mg/ml of puromycin (Calbiochem) for the selection of stable integrants. Resistant colonies were isolated and individually expanded in the absence of puromycin.

[0056] Standard Southern blotting methods were used to demonstrate stable integration of the transfected vector in puromycin-resistant clones. Briefly, genomic DNA from individual clones was prepared according to standard methods and 5-10 μg was digested with EcoRV. Digested DNA was separated in a 0.8% agarose gel and transferred to nylon membranes (GeneScreen Plus, NEN DuPont) under alkaline conditions for 16 hours. The filter was dried and hybridized for 16 hours at 65° C. with a P32-labeled probe representing the 5′ part of the E. coli beta-galactosidase gene. Hybridization was performed in a buffer containing 10% dextranesulfate, 1% SDS, 50 mM Tris and 100 mM NaCl, pH 7.5). After hybridization, the filter was washed with 2×SSC/1%SDS and exposed to BioMax MS1 X-ray films (Kodak) at −80° C.

[0057] A clone designated 3T3(pRK64)-3, which showed stable integration of pRK64, was selected for further analysis. To allow direct comparison of pCMV-C31-Int(CNLS) and pCMV-C31-Int(CNLS)-CO, the same amounts of these plasmids were introduced into 3T3(pRK64)-3 by transient transfection. Transfections were performed using the FuGene6 transfection reagent (Roche Diagnostics GmbH, Mannheim, Germany), essentially according to the manufacturers protocol. One day prior to transfections, approximately 10⁶ cells were plated into a 48-well plate. The next day, each well received 250 μl medium containing 200 ng plasmid DNA complexed to the FuGene6 transfection reagent. The 200 ng DNA preparations contained 50 ng of the luciferase expression vector pUHC13-1 (Gossen et al., Proc Natl Acad Sci USA., 89 5547-5551 (1992)), 4-32 ng of either pCMV-C31-Int(CNLS) or pCMV-C31-Int(CNLS)-CO, and pUC19 plasmid (GenBank#X02514; New England Biolabs Inc, Beverly, Mass.) to bring the total amount of DNA to 200 ng. The control sample contained 50 ng of pUHC13-1 and 150 ng pUC19. All samples contained a fixed amount of pUHC13-1 so that luciferase activity could be used to control for experimental variation of transfection and lysis. Individual preparations were tested in four replicate wells. One day after the addition of the DNA preparations, each well received additional 250 μl of growth medium. The cells of each well were lysed 48 hours after transfection with 100 μl lysis reagent supplemented with protease inhibitors (Roche Diagnostics) and centrifuged.

[0058] C. Enzyme Assays and Results

[0059] Enzyme (beta-galactosidase and luciferase) assays were performed using 20 μl lysate.

[0060] Recombination activity was measured as the level of beta-galactosidase activity (“Gal”). The beta-galactosidase chemiluminescence assay (Roche Diagnostics) was performed essentially according to the manufacturers' protocol in a Lumat LB 9507 luminometer (Berthold).

[0061] Values from the beta-galactosidase activity were normalized by luciferase activity (“Luc”). To measure luciferase activity, 20 μl lysate was diluted into 250 μl assay buffer (50 mM glycylglycin, 5 mM MgCl₂, 5 mM ATP), and the “Relative Light Units” (RLU) were counted in a Lumat LB 9507 luminometer after addition of 100 μl of a 1 mM luciferin solution (Roche Diagnostics). The mean and standard deviation for beta-galactosidase and luciferase RLU values corresponding to each DNA preparation were calculated from individual values for each of the four replicate wells. For each DNA sample, the RLU value of beta-galactosidase activity was divided by the RLU value for luciferase activity and multiplied by a factor of 10⁵. Values for enzyme activity are provided +/− standard deviations. Results of the recombination assay are shown in Table 5. TABLE 5 Results of the recombination assay. Enzyme Activity Plasmid transfected (ng) (RLU × 10⁵ pCMV-C31-Int(CNLS) pCMV-C31-Int(CNLS)-CO [Gal/Luc]) 0 0 328 +/− 281 4 0 1504 +/− 487  8 0 3085 +/− 596  16 0 3787 +/− 719  32 0 5157 +/− 798  0 4 1347 +/− 228  0 8 2453 +/− 558  0 16 3897 +/− 714  0 32 4201 +/− 715 

[0062] As shown in Table 5, the transfections with C31-Int(CNLS)-CO and C31-Int(CNLS) expression vectors resulted in comparable levels of beta-galactosidase activity. The values for 16 ng and 32 ng DNA amounts were close to saturation of the test system, as the doubling of the DNA amounts resulted only in a minor increase of recombinase activity. It was concluded that the codon-optimized C31-Int(CNLS) gene was fully functional in mammalian cells.

Example 3 Generation of Transgenic Mice Comprising the C31-Int-CO Gene

[0063] To test whether the C31-Int(CNLS)-CO gene confers enhanced C31 activity in transgenic mice, either the C31-Int(CNLS) gene or the C31-Int(CNLS)-CO gene was expressed from the identical locus in the mouse genome. The genes were inserted downstream of the ROSA26 promoter (Genbank entry gi:1778857) through homologous recombination in ES cells and chimaeric mice were generated from the recombined ES cells. These mice were mated to reporter mice carrying a C31 substrate reporter vector. Different tissues of offspring carrying the substrate vector plus one of the recombinase genes were then analysed for substrate recombination as indicated by LacZ expression.

[0064] A Vector Construction

[0065]FIG. 1 shows the ROSA26 targeting vectors for C31-Int(CNLS) (Seq ID NO: 12) and C31-Int(CNLS)-CO (Seq ID NO: 13).

[0066] The C31-Int(CNLS) and C31-Int(CNLS)-CO coding sequences were inserted downstream of a splice acceptor site (SA) such that they were expressed from the endogenous ROSA26 promoter after homologous recombination in ES cells. The coding regions were followed by a polyadenylation signal (pA) for proper transcriptional termination. An FRT-flanked selection marker conferring resistance to G418 (PGK-neo-pA) was inserted downstream. The constructs were flanked by 5′ and 3′ ROSA26 homology arms for homologous recombination in ES cells.

[0067] To generate a targeting vector for the ROSA26 locus (Friedrich, G A. and Soriano, P. (1991) Genes Dev. 5, 1513-1523), a 129 Sv/Ev-BAC library (Incyte Genomics) was screened with a probe against exon2 of the Rosa26 locus (amplified from mouse genomic DNA by PCR using Rscreen1s (SEQ ID NO:14) and Rscreen1as (SEQ ID NO:15) as primers). A BAC clone was identified, and an 11 kb EcoRV subfragment, containing the exons of the ROSA26 gene was subcloned. Of this subclone, two fragments, a 1 kb SacII/XbaI fragment (SEQ ID NO:16) and a 4 kb XbaI-fragment (SEQ ID NO:17) were used as upstream and downstream homology arms, respectively, and inserted into a vector comprising a FRT-flanked neomycin resistance gene. A splice acceptor from adenovirus site was inserted between the two homology arms and the resulting vector was designated pROSA12 (SEQ ID NO:18).

[0068] To generate the ROSA26 targeting vector for C31-Int(CNLS), the C31-Int(CNLS) coding region was inserted into pROSA12 (SEQ ID NO:18). The resulting vector was designated pROSA-SA-C31-Int(CNLS) (SEQ ID NO:12), which contained the following features as depicted in FIG. 1: an upstream homology arm for homologous recombination with the ROSA26 locus, a splice acceptor from adenovirus, the C31-Int(CNLS) coding sequence, a polyadenylation site, an FRT-flanked G418 selection cassette and the downststream ROSA26 homology arm.

[0069] The targeting vector for the C31-Int(CNLS)-CO gene was designated pROSA-SA-C31-Int(CNLS)-CO (SEQ ID NO:13) and carries the same features as the C31-Int(CNLS) targeting vector with the exception that the coding region for C31-Int(CNLS) was replaced by the C31-Int(CNLS)-CO coding region.

[0070] B. Homologous Recombination in ES Cells

[0071] The ES cell line C57B16 (Eurogentec, Belgium) was grown on mitotically inactivated feeder layer (Mitomycin C (Sigma M-0503)) comprised of mouse embryonic fibroblasts in the medium of 1×DMEM high Glucose (Invitrogen 41965-062), 2 mM Glutamin (Invitrogen 25030-024), 1× Non Essential Amino Acids (Invitrogen 11140-035) 1 mM Sodium Pyruvate (Invitrogen 11360-039), 0.1 mM β-Mercaptoethanol (Invitrogen 31350-010), 2×10⁶ u/L Leukemia Inhibitory Factor (Chemicon ESG 1107) and 20% fetal bovine serum (pre-tested for ES cell culture).

[0072] Vectors pROSA-SA-C31-Int(CNLS) or pROSA-SA-C31-Int(CNLS)-CO linearized with the restriction enzymes I-SceI or SacII, respectively, were introduced into the ES cells by electroporation. Rapidly growing cells were used one day after passaging. Upon trypsinization with 0.25% Trypsin-EDTA (Invitrogen 25200-056) cells were resuspended in PBS (Invitrogen 20012-019) and preplated for 25 min on gelatinized 10 cm plates to remove undesired feeder cells. The supernatant was harvested, ES cells were washed once in PBS and counted (Neubauer hemocytometer). 10⁷ cells were mixed with 30 μg of linearized vector in 800 μL of transfection buffer (20 mM Hepes, 137 mM NaCl, 15 mM KCl, 0.7 mM Na₂HPO₄, 6 mM Glucose 0.1 mM β-Mercaptoethanol in H₂O) and electroporated using a Biorad Gene Pulser with Capacitance Extender set on 240 V and 500 μF. Electroporated cells were seeded at a density of 2.5×10⁶ cells per 10 cm tissue culture dish onto a previously prepared layer of neomycin-resistant inactivated mouse embryonic fibroblasts.

[0073] 48 h after electroporation, the medium was replaced on all dishes by medium containing 250 μg/ml Geneticin (Invitrogen 10131-019) for positive selection of G418 resistant ES clones.

[0074] On day 8 after electroporation, ES colonies were isolated as follows:

[0075] Medium was replaced by PBS and the culture dishes were placed on the stage of a binocular (Nikon SMZ-2B). Using low magnification (25×) individual ES clones of undifferentiated appearance were removed from the surface of the culture dish by suction into the tip of a 20 μl pipette (Eppendorf). The harvested clones were placed in individual wells of 96 well plates containing 30 μL of Trypsin. After disruption of the colonies by pipetting with a multichannel pipette (Eppendorf), cells were seeded onto feeder containing 96 well plates with pre-equilibrated complete ES-medium.

[0076] Cells were grown for 3 days with daily medium changes and then split 1:2 on gelatinized (Sigma G-1890) 96 well plates. Cells were lysed 3 days after splitting, genomic DNA was prepared and analysed by Southern blot for homologous recombination. For Southern blots, genomic DNA was digested with EcoRV and separated on a 0.8% agarose gel. After transfer to a positively charged nylon membrane the samples were hybridised to probe ROSA5.1 (SEQ ID NO:19) representing sequence of the ROSA26 locus upstream of the targeting vector. The homologous recombination event was indicated by the presence of a 3.8 kb band.

[0077] C. Generation of Mice

[0078] ES cell clones carrying a single copy of the targeting vector homologously recombined in their ROSA26 locus were injected into mouse blastocysts and subsequently transferred to pseudopregnant foster mothers in order to generate chimaeras.

[0079] Balb/C male and female mice (Janvier, France) were mated to obtain blastocysts from fertilized females. Plug positive females were set aside, and 3 days later blastocysts were isolated by flushing their uteri.

[0080] For microinjection, 5-6 blastocysts were placed in a drop of DMEM with 15% FCS under mineral oil. A flat tip, piezo actuated microinjection-pipette with an internal diameter of 12-15 μm was used to inject 15 ES cells into each blastocyst. After recovery, ten injected blastocysts were transferred to each uterine horn of 2.5 days post coitum, pseudopregnant NMRI females that had been mated with vasectomized males.

[0081] After birth of the mice, high percentage chimaeras were identified by coat color chimerism.

[0082] These chimaeras were mated to heterozygous C31 reporter mice carrying the C31 substrate reporter in the ROSA26 locus (SEQ ID NO:20). FIG. 2 shows the modified ROSA26 locus of C31 reporter mice. A recombination substrate has been inserted in the ROSA26 locus. The substate has a splice acceptor (SA) followed by a cassette containing the hygromycin resistance gene driven by a PGK promoter and flanked by the recombination sites attB and attP. In addition, the reporter contains two Cre recognition sites (loxP) in direct orientation next to the att sites. This cassette is followed by the coding region for β-galactosidase, which is only expressed when the hygromycin resistance gene has been deleted by recombination.

[0083] Offspring of the crosses were genotyped for the presence of the transgenes by the following PCR assays:

[0084] PCR for C31-Int(CNLS): primers C31-1 (SEQ ID NO: 21) and C31-2 (SEQ ID NO:22) amplifying a diagnostic fragment of 500 bp. The PCR reaction contained 5 μl 10×PCR buffer (Invitrogen), 2 μl 50 mM MgCl2, 1.5 μl 10 mM dNTP-mix, 2 μl (10 pmol) of each primer, 0.5 μl Taq-polymerase (5 U/μl) and water to a volume of 50 μl. The program used for the PCR reactions was: 94° C. for 30 s, 55° C. for 30 s and 72° C. for 1 min in 30 cycles.

[0085] PCR for C31-Int(CNLS)-CO: primers were C31-h-5′ (SEQ ID NO: 23) and C31-h-3′ (SeQ ID NO:24) amplifying a 500 bp diagnostic fragment of the C31-Int(CNLS)-CO gene. The PCR reaction contained 5 μl 10×PCR buffer (Invitrogen), 2 μl 50 mM MgCl₂, 1.5 μl 10 mM dNTP-mix, 10 pmol of each primer, 2.5 U Taq polymerase in a total volume of 50 μl. PCR was performed for 30 cycles of 94° C. for 30 s, 55° C. for 1 min and 72° C. for 1 min.

[0086] PCR for ROSA26-C31 reporter allele (LacZ gene): The PCR was performed using tail DNA and the primers β-Gal 3 (SEQ ID NO:25) and β-Gal 4 (SEQ ID NO:26) amplifying a diagnostic fragment of 315 bp. The PCR reaction contained 5 μl 10×PCR buffer (Invitrogen), 2.5 μl 50 mM MgCl₂, 2 μl 10 mM dNTP-mix, 1 μl (10 pmol) of each primer, 0.4 μl Taq-polymerase (5 U/μl) and water to a volume of 50 μl. The program used for the PCR reactions was: 94° C. for 1 min, 60° C. for 1 min and 72° C. for 1 min in 30 cycles.

[0087] Tissues from mice carrying either the ROSA-C31-Int(CNLS) or the ROSA-C31-Int(CNLS)-CO targeted to the ROSA26 locus as well as the C31 substrate reporter targeted to the second ROSA26 allele and from a control mouse carrying the reporter allele only were dissected. For wholemount staining, the tissues were rinsed in 0.1 M PB (0.1 M K₂HPO₄, pH 7.3) and then fixed in fixative (0.2% glutaraldehyde, 5 mM EGTA, 2 mM MgCl₂ in 0.1 M PB) for 45 min at room temperature. They were then washed three times for 15 min at room temperature in LacZ wash buffer (2 mM MgCl₂, 0.02% Nonidet-40 in 0.1 M PB). Subsequently, the tissues were stained for beta-galactosidase activity overnight at room temperature in X-Gal solution (1 mg/ml X-Gal (predissolved in DMSO), 4 mM potassium hexacyanoferrat III, 4 mM potassium hexacyanoferrat II, in LacZ wash buffer). Tissues were washed twice for 10 min at room temperature in LacZ wash buffer and pictures were taken.

[0088] D. Results

[0089] In double transgenic mice recombination activity of the C31-Int(CNLS) recombinase was measured through activity of the beta-galactosidase produced by the recombined but not the unrecombined C31 substrate reporter. Wholemounts of the corresponding tissues from a mouse carrying only the reporter substrate were used as control. In mice carrying the ROSA-C31-Int(CNLS) knock-in plus the reporter substrate, beta-gal activity indicating recombination could not be detected in any somatic tissues, but was detected in the gonads. In contrast, mice carrying the ROSA-C31-Int(CNLS)-CO knock-in plus the reporter showed high level recombination in all tissues analysed, visible by the dark blue color of the tissues, indicating recombination of the substrate, which led to the expression of β-galactosidase.

[0090] Since both C31 genes were expressed by the same promoter from the same chromosomal location, this difference provided evidence for the superior performance of the C31-Int(CNLS)-CO sequence when integrated into a eukaryotic genome in vivo.

1 26 1 1842 DNA Bacteriophage phi-C31 1 atgacacaag gggttgtgac cggggtggac acgtacgcgg gtgcttacga ccgtcagtcg 60 cgcgagcgcg agaattcgag cgcagcaagc ccagcgacac agcgtagcgc caacgaagac 120 aaggcggccg accttcagcg cgaagtcgag cgcgacgggg gccggttcag gttcgtcggg 180 catttcagcg aagcgccggg cacgtcggcg ttcgggacgg cggagcgccc ggagttcgaa 240 cgcatcctga acgaatgccg cgccgggcgg ctcaacatga tcattgtcta tgacgtgtcg 300 cgcttctcgc gcctgaaggt catggacgcg attccgattg tctcggaatt gctcgccctg 360 ggcgtgacga ttgtttccac tcaggaaggc gtcttccggc agggaaacgt catggacctg 420 attcacctga ttatgcggct cgacgcgtcg cacaaagaat cttcgctgaa gtcggcgaag 480 attctcgaca cgaagaacct tcagcgcgaa ttgggcgggt acgtcggcgg gaaggcgcct 540 tacggcttcg agcttgtttc ggagacgaag gagatcacgc gcaacggccg aatggtcaat 600 gtcgtcatca acaagcttgc gcactcgacc actcccctta ccggaccctt cgagttcgag 660 cccgacgtaa tccggtggtg gtggcgtgag atcaagacgc acaaacacct tcccttcaag 720 ccgggcagtc aagccgccat tcacccgggc agcatcacgg ggctttgtaa gcgcatggac 780 gctgacgccg tgccgacccg gggcgagacg attgggaaga agaccgcttc aagcgcctgg 840 gacccggcaa ccgttatgcg aatccttcgg gacccgcgta ttgcgggctt cgccgctgag 900 gtgatctaca agaagaagcc ggacggcacg ccgaccacga agattgaggg ttaccgcatt 960 cagcgcgacc cgatcacgct ccggccggtc gagcttgatt gcggaccgat catcgagccc 1020 gctgagtggt atgagcttca ggcgtggttg gacggcaggg ggcgcggcaa ggggctttcc 1080 cgggggcaag ccattctgtc cgccatggac aagctgtact gcgagtgtgg cgccgtcatg 1140 acttcgaagc gcggggaaga atcgatcaag gactcttacc gctgccgtcg ccggaaggtg 1200 gtcgacccgt ccgcacctgg gcagcacgaa ggcacgtgca acgtcagcat ggcggcactc 1260 gacaagttcg ttgcggaacg catcttcaac aagatcaggc acgccgaagg cgacgaagag 1320 acgttggcgc ttctgtggga agccgcccga cgcttcggca agctcactga ggcgcctgag 1380 aagagcggcg aacgggcgaa ccttgttgcg gagcgcgccg acgccctgaa cgcccttgaa 1440 gagctgtacg aagaccgcgc ggcaggcgcg tacgacggac ccgttggcag gaagcacttc 1500 cggaagcaac aggcagcgct gacgctccgg cagcaagggg cggaagagcg gcttgccgaa 1560 cttgaagccg ccgaagcccc gaagcttccc cttgaccaat ggttccccga agacgccgac 1620 gctgacccga ccggccctaa gtcgtggtgg gggcgcgcgt cagtagacga caagcgcgtg 1680 ttcgtcgggc tcttcgtaga caagatcgtt gtcacgaagt cgactacggg cagggggcag 1740 ggaacgccca tcgagaagcg cgcttcgatc acgtgggcga agccgccgac cgacgacgac 1800 gaagacgacg cccaggacgg cacggaagac gtagcggcgt ag 1842 2 613 PRT Bacteriophage phi-C31 2 Met Thr Gln Gly Val Val Thr Gly Val Asp Thr Tyr Ala Gly Ala Tyr 1 5 10 15 Asp Arg Gln Ser Arg Glu Arg Glu Asn Ser Ser Ala Ala Ser Pro Ala 20 25 30 Thr Gln Arg Ser Ala Asn Glu Asp Lys Ala Ala Asp Leu Gln Arg Glu 35 40 45 Val Glu Arg Asp Gly Gly Arg Phe Arg Phe Val Gly His Phe Ser Glu 50 55 60 Ala Pro Gly Thr Ser Ala Phe Gly Thr Ala Glu Arg Pro Glu Phe Glu 65 70 75 80 Arg Ile Leu Asn Glu Cys Arg Ala Gly Arg Leu Asn Met Ile Ile Val 85 90 95 Tyr Asp Val Ser Arg Phe Ser Arg Leu Lys Val Met Asp Ala Ile Pro 100 105 110 Ile Val Ser Glu Leu Leu Ala Leu Gly Val Thr Ile Val Ser Thr Gln 115 120 125 Glu Gly Val Phe Arg Gln Gly Asn Val Met Asp Leu Ile His Leu Ile 130 135 140 Met Arg Leu Asp Ala Ser His Lys Glu Ser Ser Leu Lys Ser Ala Lys 145 150 155 160 Ile Leu Asp Thr Lys Asn Leu Gln Arg Glu Leu Gly Gly Tyr Val Gly 165 170 175 Gly Lys Ala Pro Tyr Gly Phe Glu Leu Val Ser Glu Thr Lys Glu Ile 180 185 190 Thr Arg Asn Gly Arg Met Val Asn Val Val Ile Asn Lys Leu Ala His 195 200 205 Ser Thr Thr Pro Leu Thr Gly Pro Phe Glu Phe Glu Pro Asp Val Ile 210 215 220 Arg Trp Trp Trp Arg Glu Ile Lys Thr His Lys His Leu Pro Phe Lys 225 230 235 240 Pro Gly Ser Gln Ala Ala Ile His Pro Gly Ser Ile Thr Gly Leu Cys 245 250 255 Lys Arg Met Asp Ala Asp Ala Val Pro Thr Arg Gly Glu Thr Ile Gly 260 265 270 Lys Lys Thr Ala Ser Ser Ala Trp Asp Pro Ala Thr Val Met Arg Ile 275 280 285 Leu Arg Asp Pro Arg Ile Ala Gly Phe Ala Ala Glu Val Ile Tyr Lys 290 295 300 Lys Lys Pro Asp Gly Thr Pro Thr Thr Lys Ile Glu Gly Tyr Arg Ile 305 310 315 320 Gln Arg Asp Pro Ile Thr Leu Arg Pro Val Glu Leu Asp Cys Gly Pro 325 330 335 Ile Ile Glu Pro Ala Glu Trp Tyr Glu Leu Gln Ala Trp Leu Asp Gly 340 345 350 Arg Gly Arg Gly Lys Gly Leu Ser Arg Gly Gln Ala Ile Leu Ser Ala 355 360 365 Met Asp Lys Leu Tyr Cys Glu Cys Gly Ala Val Met Thr Ser Lys Arg 370 375 380 Gly Glu Glu Ser Ile Lys Asp Ser Tyr Arg Cys Arg Arg Arg Lys Val 385 390 395 400 Val Asp Pro Ser Ala Pro Gly Gln His Glu Gly Thr Cys Asn Val Ser 405 410 415 Met Ala Ala Leu Asp Lys Phe Val Ala Glu Arg Ile Phe Asn Lys Ile 420 425 430 Arg His Ala Glu Gly Asp Glu Glu Thr Leu Ala Leu Leu Trp Glu Ala 435 440 445 Ala Arg Arg Phe Gly Lys Leu Thr Glu Ala Pro Glu Lys Ser Gly Glu 450 455 460 Arg Ala Asn Leu Val Ala Glu Arg Ala Asp Ala Leu Asn Ala Leu Glu 465 470 475 480 Glu Leu Tyr Glu Asp Arg Ala Ala Gly Ala Tyr Asp Gly Pro Val Gly 485 490 495 Arg Lys His Phe Arg Lys Gln Gln Ala Ala Leu Thr Leu Arg Gln Gln 500 505 510 Gly Ala Glu Glu Arg Leu Ala Glu Leu Glu Ala Ala Glu Ala Pro Lys 515 520 525 Leu Pro Leu Asp Gln Trp Phe Pro Glu Asp Ala Asp Ala Asp Pro Thr 530 535 540 Gly Pro Lys Ser Trp Trp Gly Arg Ala Ser Val Asp Asp Lys Arg Val 545 550 555 560 Phe Val Gly Leu Phe Val Asp Lys Ile Val Val Thr Lys Ser Thr Thr 565 570 575 Gly Arg Gly Gln Gly Thr Pro Ile Glu Lys Arg Ala Ser Ile Thr Trp 580 585 590 Ala Lys Pro Pro Thr Asp Asp Asp Glu Asp Asp Ala Gln Asp Gly Thr 595 600 605 Glu Asp Val Ala Ala 610 3 12 DNA Artificial Splice acceptor sequence 3 yyyyyyynca gg 12 4 12 DNA Artificial Splice acceptor site. 4 yyyyyyynta gg 12 5 1842 DNA C-31-Int-CO 5 atgacccagg gcgtggtgac cggcgtggac acctacgccg gagcctacga caggcagagc 60 agggagaggg agaacagctc cgccgccagc cccgccaccc agagatccgc caacgaggac 120 aaggccgccg acctgcagag ggaggtggag agggacggcg gcaggttcag gttcgtgggc 180 cacttcagcg aggcccccgg cacctccgcc ttcggcaccg ccgagaggcc cgagttcgag 240 aggatcctga acgagtgcag ggccggcagg ctgaacatga tcatcgtgta cgatgtgagc 300 aggttcagca ggctgaaggt catggatgcc atccccatcg tgtccgagct gctggccctg 360 ggcgtgacca tcgtgagcac ccaggagggc gtgttcaggc agggcaacgt gatggacctg 420 atccacctga tcatgaggct ggatgccagc cacaaggaga gcagcctgaa gtccgccaag 480 atcctggaca ccaagaacct gcagagagag ctgggcggct acgtgggcgg caaggccccc 540 tacggcttcg aactcgtgag cgagaccaag gagatcacca ggaacggcag gatggtgaac 600 gtggtgatca acaagctggc ccacagcacc acccccctga ccggcccctt cgagttcgag 660 cccgacgtga tcaggtggtg gtggagggag atcaagaccc acaagcacct gcccttcaag 720 cccggcagcc aggccgccat ccaccccggc agcatcaccg gcctgtgcaa gaggatggat 780 gccgatgccg tgcccaccag gggcgagacc atcggcaaga aaaccgccag ctccgcctgg 840 gaccccgcca ccgtgatgag gatcctgagg gacccccgga tcgccggctt cgccgccgag 900 gtgatctaca agaagaagcc cgacggcacc cccaccacca agatcgaggg ctacaggatc 960 cagagggacc ccatcaccct gaggcccgtg gagctggact gcggccccat catcgagccc 1020 gccgagtggt acgagctgca ggcctggctg gacggcaggg gcaggggcaa gggcctgagc 1080 aggggccagg ccatcctgtc cgccatggac aagctgtact gcgagtgcgg agccgtgatg 1140 accagcaaga ggggcgagga gagcatcaag gacagctaca gatgcaggag gaggaaggtg 1200 gtggacccct ccgcccccgg ccagcacgag ggcacctgca acgtgagcat ggccgccctg 1260 gacaagttcg tggccgagag gatcttcaac aagatcaggc acgccgaggg cgacgaggag 1320 accctggccc tgctgtggga ggccgccagg aggttcggca agctgaccga ggcccccgag 1380 aagagcggcg agagggccaa cctggtggcc gagagggccg atgccctgaa tgccctggag 1440 gagctgtacg aggacagggc cgccggagcc tacgacggcc ccgtgggcag gaagcacttc 1500 aggaagcagc aggccgccct gaccctgagg cagcagggag ccgaggagag gctggccgag 1560 ctggaggccg ccgaggcccc caagctgccc ctggaccagt ggttccccga ggatgccgat 1620 gccgacccca ccggccccaa gagctggtgg ggcagggcca gcgtggacga caagagggtg 1680 ttcgtgggcc tgttcgtgga caagatcgtg gtgaccaaga gcaccaccgg caggggccag 1740 ggcaccccca tcgagaagag ggccagcatc acctgggcca agccccccac cgacgacgac 1800 gaggacgatg cccaggacgg caccgaggac gtggccgcct ga 1842 6 1863 DNA C-31-Int-(CNLS) 6 atgacccagg gcgtggtgac cggcgtggac acctacgccg gagcctacga caggcagagc 60 agggagaggg agaacagctc cgccgccagc cccgccaccc agagatccgc caacgaggac 120 aaggccgccg acctgcagag ggaggtggag agggacggcg gcaggttcag gttcgtgggc 180 cacttcagcg aggcccccgg cacctccgcc ttcggcaccg ccgagaggcc cgagttcgag 240 aggatcctga acgagtgcag ggccggcagg ctgaacatga tcatcgtgta cgatgtgagc 300 aggttcagca ggctgaaggt catggatgcc atccccatcg tgtccgagct gctggccctg 360 ggcgtgacca tcgtgagcac ccaggagggc gtgttcaggc agggcaacgt gatggacctg 420 atccacctga tcatgaggct ggatgccagc cacaaggaga gcagcctgaa gtccgccaag 480 atcctggaca ccaagaacct gcagagagag ctgggcggct acgtgggcgg caaggccccc 540 tacggcttcg aactcgtgag cgagaccaag gagatcacca ggaacggcag gatggtgaac 600 gtggtgatca acaagctggc ccacagcacc acccccctga ccggcccctt cgagttcgag 660 cccgacgtga tcaggtggtg gtggagggag atcaagaccc acaagcacct gcccttcaag 720 cccggcagcc aggccgccat ccaccccggc agcatcaccg gcctgtgcaa gaggatggat 780 gccgatgccg tgcccaccag gggcgagacc atcggcaaga aaaccgccag ctccgcctgg 840 gaccccgcca ccgtgatgag gatcctgagg gacccccgga tcgccggctt cgccgccgag 900 gtgatctaca agaagaagcc cgacggcacc cccaccacca agatcgaggg ctacaggatc 960 cagagggacc ccatcaccct gaggcccgtg gagctggact gcggccccat catcgagccc 1020 gccgagtggt acgagctgca ggcctggctg gacggcaggg gcaggggcaa gggcctgagc 1080 aggggccagg ccatcctgtc cgccatggac aagctgtact gcgagtgcgg agccgtgatg 1140 accagcaaga ggggcgagga gagcatcaag gacagctaca gatgcaggag gaggaaggtg 1200 gtggacccct ccgcccccgg ccagcacgag ggcacctgca acgtgagcat ggccgccctg 1260 gacaagttcg tggccgagag gatcttcaac aagatcaggc acgccgaggg cgacgaggag 1320 accctggccc tgctgtggga ggccgccagg aggttcggca agctgaccga ggcccccgag 1380 aagagcggcg agagggccaa cctggtggcc gagagggccg atgccctgaa tgccctggag 1440 gagctgtacg aggacagggc cgccggagcc tacgacggcc ccgtgggcag gaagcacttc 1500 aggaagcagc aggccgccct gaccctgagg cagcagggag ccgaggagag gctggccgag 1560 ctggaggccg ccgaggcccc caagctgccc ctggaccagt ggttccccga ggatgccgat 1620 gccgacccca ccggccccaa gagctggtgg ggcagggcca gcgtggacga caagagggtg 1680 ttcgtgggcc tgttcgtgga caagatcgtg gtgaccaaga gcaccaccgg caggggccag 1740 ggcaccccca tcgagaagag ggccagcatc acctgggcca agccccccac cgacgacgac 1800 gaggacgatg cccaggacgg caccgaggac gtggccgccc ccaagaagaa gaggaaggtg 1860 tga 1863 7 620 PRT C-31-Int-(CNLS) 7 Met Thr Gln Gly Val Val Thr Gly Val Asp Thr Tyr Ala Gly Ala Tyr 1 5 10 15 Asp Arg Gln Ser Arg Glu Arg Glu Asn Ser Ser Ala Ala Ser Pro Ala 20 25 30 Thr Gln Arg Ser Ala Asn Glu Asp Lys Ala Ala Asp Leu Gln Arg Glu 35 40 45 Val Glu Arg Asp Gly Gly Arg Phe Arg Phe Val Gly His Phe Ser Glu 50 55 60 Ala Pro Gly Thr Ser Ala Phe Gly Thr Ala Glu Arg Pro Glu Phe Glu 65 70 75 80 Arg Ile Leu Asn Glu Cys Arg Ala Gly Arg Leu Asn Met Ile Ile Val 85 90 95 Tyr Asp Val Ser Arg Phe Ser Arg Leu Lys Val Met Asp Ala Ile Pro 100 105 110 Ile Val Ser Glu Leu Leu Ala Leu Gly Val Thr Ile Val Ser Thr Gln 115 120 125 Glu Gly Val Phe Arg Gln Gly Asn Val Met Asp Leu Ile His Leu Ile 130 135 140 Met Arg Leu Asp Ala Ser His Lys Glu Ser Ser Leu Lys Ser Ala Lys 145 150 155 160 Ile Leu Asp Thr Lys Asn Leu Gln Arg Glu Leu Gly Gly Tyr Val Gly 165 170 175 Gly Lys Ala Pro Tyr Gly Phe Glu Leu Val Ser Glu Thr Lys Glu Ile 180 185 190 Thr Arg Asn Gly Arg Met Val Asn Val Val Ile Asn Lys Leu Ala His 195 200 205 Ser Thr Thr Pro Leu Thr Gly Pro Phe Glu Phe Glu Pro Asp Val Ile 210 215 220 Arg Trp Trp Trp Arg Glu Ile Lys Thr His Lys His Leu Pro Phe Lys 225 230 235 240 Pro Gly Ser Gln Ala Ala Ile His Pro Gly Ser Ile Thr Gly Leu Cys 245 250 255 Lys Arg Met Asp Ala Asp Ala Val Pro Thr Arg Gly Glu Thr Ile Gly 260 265 270 Lys Lys Thr Ala Ser Ser Ala Trp Asp Pro Ala Thr Val Met Arg Ile 275 280 285 Leu Arg Asp Pro Arg Ile Ala Gly Phe Ala Ala Glu Val Ile Tyr Lys 290 295 300 Lys Lys Pro Asp Gly Thr Pro Thr Thr Lys Ile Glu Gly Tyr Arg Ile 305 310 315 320 Gln Arg Asp Pro Ile Thr Leu Arg Pro Val Glu Leu Asp Cys Gly Pro 325 330 335 Ile Ile Glu Pro Ala Glu Trp Tyr Glu Leu Gln Ala Trp Leu Asp Gly 340 345 350 Arg Gly Arg Gly Lys Gly Leu Ser Arg Gly Gln Ala Ile Leu Ser Ala 355 360 365 Met Asp Lys Leu Tyr Cys Glu Cys Gly Ala Val Met Thr Ser Lys Arg 370 375 380 Gly Glu Glu Ser Ile Lys Asp Ser Tyr Arg Cys Arg Arg Arg Lys Val 385 390 395 400 Val Asp Pro Ser Ala Pro Gly Gln His Glu Gly Thr Cys Asn Val Ser 405 410 415 Met Ala Ala Leu Asp Lys Phe Val Ala Glu Arg Ile Phe Asn Lys Ile 420 425 430 Arg His Ala Glu Gly Asp Glu Glu Thr Leu Ala Leu Leu Trp Glu Ala 435 440 445 Ala Arg Arg Phe Gly Lys Leu Thr Glu Ala Pro Glu Lys Ser Gly Glu 450 455 460 Arg Ala Asn Leu Val Ala Glu Arg Ala Asp Ala Leu Asn Ala Leu Glu 465 470 475 480 Glu Leu Tyr Glu Asp Arg Ala Ala Gly Ala Tyr Asp Gly Pro Val Gly 485 490 495 Arg Lys His Phe Arg Lys Gln Gln Ala Ala Leu Thr Leu Arg Gln Gln 500 505 510 Gly Ala Glu Glu Arg Leu Ala Glu Leu Glu Ala Ala Glu Ala Pro Lys 515 520 525 Leu Pro Leu Asp Gln Trp Phe Pro Glu Asp Ala Asp Ala Asp Pro Thr 530 535 540 Gly Pro Lys Ser Trp Trp Gly Arg Ala Ser Val Asp Asp Lys Arg Val 545 550 555 560 Phe Val Gly Leu Phe Val Asp Lys Ile Val Val Thr Lys Ser Thr Thr 565 570 575 Gly Arg Gly Gln Gly Thr Pro Ile Glu Lys Arg Ala Ser Ile Thr Trp 580 585 590 Ala Lys Pro Pro Thr Asp Asp Asp Glu Asp Asp Ala Gln Asp Gly Thr 595 600 605 Glu Asp Val Ala Ala Pro Lys Lys Lys Arg Lys Val 610 615 620 8 1885 DNA C-31-Int-(CNLS)-CO 8 gatatcgcca ccatgaccca gggcgtggtg accggcgtgg acacctacgc cggagcctac 60 gacaggcaga gcagggagag ggagaacagc tccgccgcca gccccgccac ccagagatcc 120 gccaacgagg acaaggccgc cgacctgcag agggaggtgg agagggacgg cggcaggttc 180 aggttcgtgg gccacttcag cgaggccccc ggcacctccg ccttcggcac cgccgagagg 240 cccgagttcg agaggatcct gaacgagtgc agggccggca ggctgaacat gatcatcgtg 300 tacgatgtga gcaggttcag caggctgaag gtcatggatg ccatccccat cgtgtccgag 360 ctgctggccc tgggcgtgac catcgtgagc acccaggagg gcgtgttcag gcagggcaac 420 gtgatggacc tgatccacct gatcatgagg ctggatgcca gccacaagga gagcagcctg 480 aagtccgcca agatcctgga caccaagaac ctgcagagag agctgggcgg ctacgtgggc 540 ggcaaggccc cctacggctt cgaactcgtg agcgagacca aggagatcac caggaacggc 600 aggatggtga acgtggtgat caacaagctg gcccacagca ccacccccct gaccggcccc 660 ttcgagttcg agcccgacgt gatcaggtgg tggtggaggg agatcaagac ccacaagcac 720 ctgcccttca agcccggcag ccaggccgcc atccaccccg gcagcatcac cggcctgtgc 780 aagaggatgg atgccgatgc cgtgcccacc aggggcgaga ccatcggcaa gaaaaccgcc 840 agctccgcct gggaccccgc caccgtgatg aggatcctga gggacccccg gatcgccggc 900 ttcgccgccg aggtgatcta caagaagaag cccgacggca cccccaccac caagatcgag 960 ggctacagga tccagaggga ccccatcacc ctgaggcccg tggagctgga ctgcggcccc 1020 atcatcgagc ccgccgagtg gtacgagctg caggcctggc tggacggcag gggcaggggc 1080 aagggcctga gcaggggcca ggccatcctg tccgccatgg acaagctgta ctgcgagtgc 1140 ggagccgtga tgaccagcaa gaggggcgag gagagcatca aggacagcta cagatgcagg 1200 aggaggaagg tggtggaccc ctccgccccc ggccagcacg agggcacctg caacgtgagc 1260 atggccgccc tggacaagtt cgtggccgag aggatcttca acaagatcag gcacgccgag 1320 ggcgacgagg agaccctggc cctgctgtgg gaggccgcca ggaggttcgg caagctgacc 1380 gaggcccccg agaagagcgg cgagagggcc aacctggtgg ccgagagggc cgatgccctg 1440 aatgccctgg aggagctgta cgaggacagg gccgccggag cctacgacgg ccccgtgggc 1500 aggaagcact tcaggaagca gcaggccgcc ctgaccctga ggcagcaggg agccgaggag 1560 aggctggccg agctggaggc cgccgaggcc cccaagctgc ccctggacca gtggttcccc 1620 gaggatgccg atgccgaccc caccggcccc aagagctggt ggggcagggc cagcgtggac 1680 gacaagaggg tgttcgtggg cctgttcgtg gacaagatcg tggtgaccaa gagcaccacc 1740 ggcaggggcc agggcacccc catcgagaag agggccagca tcacctgggc caagcccccc 1800 accgacgacg acgaggacga tgcccaggac ggcaccgagg acgtggccgc ccccaagaag 1860 aagaggaagg tgtgatgaag atatc 1885 9 5723 DNA pCMV-C31-Int(CNLS) 9 ggcacgacag gtttcccgac tggaaagcgg gcagtgagcg caacgcaatt aatgtgagtt 60 agctcactca ttaggcaccc caggctttac actttatgct tccggctcgt atgttgtgtg 120 gaattgtgag cggataacaa tttcacacag gaaacagcta tgaccatgat tacgccaagc 180 tagcccgggc tagcttgcat gcctgcaggt ttaaacagtc cgatgtacgg gccagatata 240 cgcgttgaca ttgattattg actagttatt aatagtaatc aattacgggg tcattagttc 300 atagcccata tatggagttc cgcgttacat aacttacggt aaatggcccg cctggctgac 360 cgcccaacga cccccgccca ttgacgtcaa taatgacgta tgttcccata gtaacgccaa 420 tagggacttt ccattgacgt caatgggtgg actatttacg gtaaactgcc cacttggcag 480 tacatcaagt gtatcatatg ccaagtacgc cccctattga cgtcaatgac ggtaaatggc 540 ccgcctggca ttatgcccag tacatgacct tatgggactt tcctacttgg cagtacatct 600 acgtattagt catcgctatt accatggtga tgcggttttg gcagtacatc aatgggcgtg 660 gatagcggtt tgactcacgg ggatttccaa gtctccaccc cattgacgtc aatgggagtt 720 tgttttggca ccaaaatcaa cgggactttc caaaatgtcg taacaactcc gccccattga 780 cgcaaatggg cggtaggcgt gtacggtggg aggtctatat aagcagagct ctctggctaa 840 ctagagaacc cactgcttac tggcttatcg aaattaatac gactcactat agggagaccc 900 aagctgactc tagacttaat taagcgttgg ggtgagtact ccctctcaaa agcgggcatg 960 acttctgcgc taagattgtc agtttccaaa aacgaggagg atttgatatt cacctggccc 1020 gcggtgatgc ctttgagggt ggccgcgtcc atctggtcag aaaagacaat ctttttgttg 1080 tcaagcttga ggtgtggcag gcttgagatc tggccataca cttgagtgac attgacatcc 1140 actttgcctt tctctccaca ggtgtccact cccagggcgg ccgcccgata tgacacaagg 1200 ggttgtgacc ggggtggaca cgtacgcggg tgcttacgac cgtcagtcgc gcgagcgcga 1260 gaattcgagc gcagcaagcc cagcgacaca gcgtagcgcc aacgaagaca aggcggccga 1320 ccttcagcgc gaagtcgagc gcgacggggg ccggttcagg ttcgtcgggc atttcagcga 1380 agcgccgggc acgtcggcgt tcgggacggc ggagcgcccg gagttcgaac gcatcctgaa 1440 cgaatgccgc gccgggcggc tcaacatgat cattgtctat gacgtgtcgc gcttctcgcg 1500 cctgaaggtc atggacgcga ttccgattgt ctcggaattg ctcgccctgg gcgtgacgat 1560 tgtttccact caggaaggcg tcttccggca gggaaacgtc atggacctga ttcacctgat 1620 tatgcggctc gacgcgtcgc acaaagaatc ttcgctgaag tcggcgaaga ttctcgacac 1680 gaagaacctt cagcgcgaat tgggcgggta cgtcggcggg aaggcgcctt acggcttcga 1740 gcttgtttcg gagacgaagg agatcacgcg caacggccga atggtcaatg tcgtcatcaa 1800 caagcttgcg cactcgacca ctccccttac cggacccttc gagttcgagc ccgacgtaat 1860 ccggtggtgg tggcgtgaga tcaagacgca caaacacctt cccttcaagc cgggcagtca 1920 agccgccatt cacccgggca gcatcacggg gctttgtaag cgcatggacg ctgacgccgt 1980 gccgacccgg ggcgagacga ttgggaagaa gaccgcttca agcgcctggg acccggcaac 2040 cgttatgcga atccttcggg acccgcgtat tgcgggcttc gccgctgagg tgatctacaa 2100 gaagaagccg gacggcacgc cgaccacgaa gattgagggt taccgcattc agcgcgaccc 2160 gatcacgctc cggccggtcg agcttgattg cggaccgatc atcgagcccg ctgagtggta 2220 tgagcttcag gcgtggttgg acggcagggg gcgcggcaag gggctttccc gggggcaagc 2280 cattctgtcc gccatggaca agctgtactg cgagtgtggc gccgtcatga cttcgaagcg 2340 cggggaagaa tcgatcaagg actcttaccg ctgccgtcgc cggaaggtgg tcgacccgtc 2400 cgcacctggg cagcacgaag gcacgtgcaa cgtcagcatg gcggcactcg acaagttcgt 2460 tgcggaacgc atcttcaaca agatcaggca cgccgaaggc gacgaagaga cgttggcgct 2520 tctgtgggaa gccgcccgac gcttcggcaa gctcactgag gcgcctgaga agagcggcga 2580 acgggcgaac cttgttgcgg agcgcgccga cgccctgaac gcccttgaag agctgtacga 2640 agaccgcgcg gcaggcgcgt acgacggacc cgttggcagg aagcacttcc ggaagcaaca 2700 ggcagcgctg acgctccggc agcaaggggc ggaagagcgg cttgccgaac ttgaagccgc 2760 cgaagccccg aagcttcccc ttgaccaatg gttccccgaa gacgccgacg ctgacccgac 2820 cggccctaag tcgtggtggg ggcgcgcgtc agtagacgac aagcgcgtgt tcgtcgggct 2880 cttcgtagac aagatcgttg tcacgaagtc gactacgggc agggggcagg gaacgcccat 2940 cgagaagcgc gcttcgatca cgtgggcgaa gccgccgacc gacgacgacg aagacgacgc 3000 ccaggacggc acggaagacg tagcggcgcc taagaagaag aggaaggttt agactctcga 3060 gatccaggcg cggatcaata aaagatcatt attttcaata gatctgtgtg ttggtttttt 3120 gtgtgccttg ggggaggggg aggccagaat gaggcgcggc caagggggag ggggaggcca 3180 gaatgacctt gggggagggg gaggccagaa tgaccttggg ggagggggag gccagaatga 3240 ggcgcgcccc cgggtaccga gctcgaattc actggccgtc gttttacaac gtcgtgactg 3300 ggaaaaccct ggcgttaccc aacttaatcg ccttgcagca catccccctt tcgccagctg 3360 gcgtaatagc gaagaggccc gcaccgatcg cccttcccaa cagttgcgca gcctgaatgg 3420 cgaatggcgc ctgatgcggt attttctcct tacgcatctg tgcggtattt cacaccgcat 3480 atggtgcact ctcagtacaa tctgctctga tgccgcatag ttaagccagc cccgacaccc 3540 gccaacaccc gctgacgcgc cctgacgggc ttgtctgctc ccggcatccg cttacagaca 3600 agctgtgacc gtctccggga gctgcatgtg tcagaggttt tcaccgtcat caccgaaacg 3660 cgcgagacga aagggcctcg tgatacgcct atttttatag gttaatgtca tgataataat 3720 ggtttcttag acgtcaggtg gcacttttcg gggaaatgtg cgcggaaccc ctatttgttt 3780 atttttctaa atacattcaa atatgtatcc gctcatgaga caataaccct gataaatgct 3840 tcaataatat tgaaaaagga agagtatgag tattcaacat ttccgtgtcg cccttattcc 3900 cttttttgcg gcattttgcc ttcctgtttt tgctcaccca gaaacgctgg tgaaagtaaa 3960 agatgctgaa gatcagttgg gtgcacgagt gggttacatc gaactggatc tcaacagcgg 4020 taagatcctt gagagttttc gccccgaaga acgttttcca atgatgagca cttttaaagt 4080 tctgctatgt ggcgcggtat tatcccgtat tgacgccggg caagagcaac tcggtcgccg 4140 catacactat tctcagaatg acttggttga gtactcacca gtcacagaaa agcatcttac 4200 ggatggcatg acagtaagag aattatgcag tgctgccata accatgagtg ataacactgc 4260 ggccaactta cttctgacaa cgatcggagg accgaaggag ctaaccgctt ttttgcacaa 4320 catgggggat catgtaactc gccttgatcg ttgggaaccg gagctgaatg aagccatacc 4380 aaacgacgag cgtgacacca cgatgcctgt agcaatggca acaacgttgc gcaaactatt 4440 aactggcgaa ctacttactc tagcttcccg gcaacaatta atagactgga tggaggcgga 4500 taaagttgca ggaccacttc tgcgctcggc ccttccggct ggctggttta ttgctgataa 4560 atctggagcc ggtgagcgtg ggtctcgcgg tatcattgca gcactggggc cagatggtaa 4620 gccctcccgt atcgtagtta tctacacgac ggggagtcag gcaactatgg atgaacgaaa 4680 tagacagatc gctgagatag gtgcctcact gattaagcat tggtaactgt cagaccaagt 4740 ttactcatat atactttaga ttgatttaaa acttcatttt taatttaaaa ggatctaggt 4800 gaagatcctt tttgataatc tcatgaccaa aatcccttaa cgtgagtttt cgttccactg 4860 agcgtcagac cccgtagaaa agatcaaagg atcttcttga gatccttttt ttctgcgcgt 4920 aatctgctgc ttgcaaacaa aaaaaccacc gctaccagcg gtggtttgtt tgccggatca 4980 agagctacca actctttttc cgaaggtaac tggcttcagc agagcgcaga taccaaatac 5040 tgtccttcta gtgtagccgt agttaggcca ccacttcaag aactctgtag caccgcctac 5100 atacctcgct ctgctaatcc tgttaccagt ggctgctgcc agtggcgata agtcgtgtct 5160 taccgggttg gactcaagac gatagttacc ggataaggcg cagcggtcgg gctgaacggg 5220 gggttcgtgc acacagccca gcttggagcg aacgacctac accgaactga gatacctaca 5280 gcgtgagcta tgagaaagcg ccacgcttcc cgaagggaga aaggcggaca ggtatccggt 5340 aagcggcagg gtcggaacag gagagcgcac gagggagctt ccagggggaa acgcctggta 5400 tctttatagt cctgtcgggt ttcgccacct ctgacttgag cgtcgatttt tgtgatgctc 5460 gtcagggggg cggagcctat ggaaaaacgc cagcaacgcg gcctttttac ggttcctggc 5520 cttttgctgg ccttttgctc acatgttctt tcctgcgtta tcccctgatt ctgtggataa 5580 ccgtattacc gcctttgagt gagctgatac cgctcgccgc agccgaacga ccgagcgcag 5640 cgagtcagtg agcgaggaag cggaagagcg cccaatacgc aaaccgcctc tccccgcgcg 5700 ttggccgatt cattaatgca gct 5723 10 5741 DNA pCMV-C31-Ins(CNLS)-CO 10 ggccagcgtg gacgacaaga gggtgttcgt gggcctgttc gtggacaaga tcgtggtgac 60 caagagcacc accggcaggg gccagggcac ccccatcgag aagagggcca gcatcacctg 120 ggccaagccc cccaccgacg acgacgagga cgatgcccag gacggcaccg aggacgtggc 180 cgcccccaag aagaagagga aggtgtgatg aagatggccg cgtcgacctc gagatccagg 240 cgcggatcaa taaaagatca ttattttcaa tagatctgtg tgttggtttt ttgtgtgcct 300 tgggggaggg ggaggccaga atgaggcgcg gccaaggggg agggggaggc cagaatgacc 360 ttgggggagg gggaggccag aatgaccttg ggggaggggg aggccagaat gaggcgcgcc 420 cccgggtacc gagctcgaat tcactggccg tcgttttaca acgtcgtgac tgggaaaacc 480 ctggcgttac ccaacttaat cgccttgcag cacatccccc tttcgccagc tggcgtaata 540 gcgaagaggc ccgcaccgat cgcccttccc aacagttgcg cagcctgaat ggcgaatggc 600 gcctgatgcg gtattttctc cttacgcatc tgtgcggtat ttcacaccgc atatggtgca 660 ctctcagtac aatctgctct gatgccgcat agttaagcca gccccgacac ccgccaacac 720 ccgctgacgc gccctgacgg gcttgtctgc tcccggcatc cgcttacaga caagctgtga 780 ccgtctccgg gagctgcatg tgtcagaggt tttcaccgtc atcaccgaaa cgcgcgagac 840 gaaagggcct cgtgatacgc ctatttttat aggttaatgt catgataata atggtttctt 900 agacgtcagg tggcactttt cggggaaatg tgcgcggaac ccctatttgt ttatttttct 960 aaatacattc aaatatgtat ccgctcatga gacaataacc ctgataaatg cttcaataat 1020 attgaaaaag gaagagtatg agtattcaac atttccgtgt cgcccttatt cccttttttg 1080 cggcattttg ccttcctgtt tttgctcacc cagaaacgct ggtgaaagta aaagatgctg 1140 aagatcagtt gggtgcacga gtgggttaca tcgaactgga tctcaacagc ggtaagatcc 1200 ttgagagttt tcgccccgaa gaacgttttc caatgatgag cacttttaaa gttctgctat 1260 gtggcgcggt attatcccgt attgacgccg ggcaagagca actcggtcgc cgcatacact 1320 attctcagaa tgacttggtt gagtactcac cagtcacaga aaagcatctt acggatggca 1380 tgacagtaag agaattatgc agtgctgcca taaccatgag tgataacact gcggccaact 1440 tacttctgac aacgatcgga ggaccgaagg agctaaccgc ttttttgcac aacatggggg 1500 atcatgtaac tcgccttgat cgttgggaac cggagctgaa tgaagccata ccaaacgacg 1560 agcgtgacac cacgatgcct gtagcaatgg caacaacgtt gcgcaaacta ttaactggcg 1620 aactacttac tctagcttcc cggcaacaat taatagactg gatggaggcg gataaagttg 1680 caggaccact tctgcgctcg gcccttccgg ctggctggtt tattgctgat aaatctggag 1740 ccggtgagcg tgggtctcgc ggtatcattg cagcactggg gccagatggt aagccctccc 1800 gtatcgtagt tatctacacg acggggagtc aggcaactat ggatgaacga aatagacaga 1860 tcgctgagat aggtgcctca ctgattaagc attggtaact gtcagaccaa gtttactcat 1920 atatacttta gattgattta aaacttcatt tttaatttaa aaggatctag gtgaagatcc 1980 tttttgataa tctcatgacc aaaatccctt aacgtgagtt ttcgttccac tgagcgtcag 2040 accccgtaga aaagatcaaa ggatcttctt gagatccttt ttttctgcgc gtaatctgct 2100 gcttgcaaac aaaaaaacca ccgctaccag cggtggtttg tttgccggat caagagctac 2160 caactctttt tccgaaggta actggcttca gcagagcgca gataccaaat actgtccttc 2220 tagtgtagcc gtagttaggc caccacttca agaactctgt agcaccgcct acatacctcg 2280 ctctgctaat cctgttacca gtggctgctg ccagtggcga taagtcgtgt cttaccgggt 2340 tggactcaag acgatagtta ccggataagg cgcagcggtc gggctgaacg gggggttcgt 2400 gcacacagcc cagcttggag cgaacgacct acaccgaact gagataccta cagcgtgagc 2460 tatgagaaag cgccacgctt cccgaaggga gaaaggcgga caggtatccg gtaagcggca 2520 gggtcggaac aggagagcgc acgagggagc ttccaggggg aaacgcctgg tatctttata 2580 gtcctgtcgg gtttcgccac ctctgacttg agcgtcgatt tttgtgatgc tcgtcagggg 2640 ggcggagcct atggaaaaac gccagcaacg cggccttttt acggttcctg gccttttgct 2700 ggccttttgc tcacatgttc tttcctgcgt tatcccctga ttctgtggat aaccgtatta 2760 ccgcctttga gtgagctgat accgctcgcc gcagccgaac gaccgagcgc agcgagtcag 2820 tgagcgagga agcggaagag cgcccaatac gcaaaccgcc tctccccgcg cgttggccga 2880 ttcattaatg cagctggcac gacaggtttc ccgactggaa agcgggcagt gagcgcaacg 2940 caattaatgt gagttagctc actcattagg caccccaggc tttacacttt atgcttccgg 3000 ctcgtatgtt gtgtggaatt gtgagcggat aacaatttca cacaggaaac agctatgacc 3060 atgattacgc caagctagcc cgggctagct tgcatgcctg caggtttaaa cagtccgatg 3120 tacgggccag atatacgcgt tgacattgat tattgactag ttattaatag taatcaatta 3180 cggggtcatt agttcatagc ccatatatgg agttccgcgt tacataactt acggtaaatg 3240 gcccgcctgg ctgaccgccc aacgaccccc gcccattgac gtcaataatg acgtatgttc 3300 ccatagtaac gccaataggg actttccatt gacgtcaatg ggtggactat ttacggtaaa 3360 ctgcccactt ggcagtacat caagtgtatc atatgccaag tacgccccct attgacgtca 3420 atgacggtaa atggcccgcc tggcattatg cccagtacat gaccttatgg gactttccta 3480 cttggcagta catctacgta ttagtcatcg ctattaccat ggtgatgcgg ttttggcagt 3540 acatcaatgg gcgtggatag cggtttgact cacggggatt tccaagtctc caccccattg 3600 acgtcaatgg gagtttgttt tggcaccaaa atcaacggga ctttccaaaa tgtcgtaaca 3660 actccgcccc attgacgcaa atgggcggta ggcgtgtacg gtgggaggtc tatataagca 3720 gagctctctg gctaactaga gaacccactg cttactggct tatcgaaatt aatacgactc 3780 actataggga gacccaagct gactctagac ttaattaagc gttggggtga gtactccctc 3840 tcaaaagcgg gcatgacttc tgcgctaaga ttgtcagttt ccaaaaacga ggaggatttg 3900 atattcacct ggcccgcggt gatgcctttg agggtggccg cgtccatctg gtcagaaaag 3960 acaatctttt tgttgtcaag cttgaggtgt ggcaggcttg agatctggcc atacacttga 4020 gtgacattga catccacttt gcctttctct ccacaggtgt ccactcccag ggcggccatc 4080 gccaccatga cccagggcgt ggtgaccggc gtggacacct acgccggagc ctacgacagg 4140 cagagcaggg agagggagaa cagctccgcc gccagccccg ccacccagag atccgccaac 4200 gaggacaagg ccgccgacct gcagagggag gtggagaggg acggcggcag gttcaggttc 4260 gtgggccact tcagcgaggc ccccggcacc tccgccttcg gcaccgccga gaggcccgag 4320 ttcgagagga tcctgaacga gtgcagggcc ggcaggctga acatgatcat cgtgtacgat 4380 gtgagcaggt tcagcaggct gaaggtcatg gatgccatcc ccatcgtgtc cgagctgctg 4440 gccctgggcg tgaccatcgt gagcacccag gagggcgtgt tcaggcaggg caacgtgatg 4500 gacctgatcc acctgatcat gaggctggat gccagccaca aggagagcag cctgaagtcc 4560 gccaagatcc tggacaccaa gaacctgcag agagagctgg gcggctacgt gggcggcaag 4620 gccccctacg gcttcgaact cgtgagcgag accaaggaga tcaccaggaa cggcaggatg 4680 gtgaacgtgg tgatcaacaa gctggcccac agcaccaccc ccctgaccgg ccccttcgag 4740 ttcgagcccg acgtgatcag gtggtggtgg agggagatca agacccacaa gcacctgccc 4800 ttcaagcccg gcagccaggc cgccatccac cccggcagca tcaccggcct gtgcaagagg 4860 atggatgccg atgccgtgcc caccaggggc gagaccatcg gcaagaaaac cgccagctcc 4920 gcctgggacc ccgccaccgt gatgaggatc ctgagggacc cccggatcgc cggcttcgcc 4980 gccgaggtga tctacaagaa gaagcccgac ggcaccccca ccaccaagat cgagggctac 5040 aggatccaga gggaccccat caccctgagg cccgtggagc tggactgcgg ccccatcatc 5100 gagcccgccg agtggtacga gctgcaggcc tggctggacg gcaggggcag gggcaagggc 5160 ctgagcaggg gccaggccat cctgtccgcc atggacaagc tgtactgcga gtgcggagcc 5220 gtgatgacca gcaagagggg cgaggagagc atcaaggaca gctacagatg caggaggagg 5280 aaggtggtgg acccctccgc ccccggccag cacgagggca cctgcaacgt gagcatggcc 5340 gccctggaca agttcgtggc cgagaggatc ttcaacaaga tcaggcacgc cgagggcgac 5400 gaggagaccc tggccctgct gtgggaggcc gccaggaggt tcggcaagct gaccgaggcc 5460 cccgagaaga gcggcgagag ggccaacctg gtggccgaga gggccgatgc cctgaatgcc 5520 ctggaggagc tgtacgagga cagggccgcc ggagcctacg acggccccgt gggcaggaag 5580 cacttcagga agcagcaggc cgccctgacc ctgaggcagc agggagccga ggagaggctg 5640 gccgagctgg aggccgccga ggcccccaag ctgcccctgg accagtggtt ccccgaggat 5700 gccgatgccg accccaccgg ccccaagagc tggtggggca g 5741 11 7438 DNA pRK64 11 cgtcatcacc gaaacgcgcg aggcagctgt ggaatgtgtg tcagttaggg tgtggaaagt 60 ccccaggctc cccagcaggc agaagtatgc aaagcatgca tctcaattag tcagcaacca 120 ggctccccag caggcagaag tgtgcaaagc atgcatctca attagtcagc aaccatagtc 180 ccgcccctaa ctccgcccat cccgccccta actccgccca gttccgccca ttctccgccc 240 catggctgac taattttttt tatttatgca gaggccgagg ccgcctcggc ctaggaacag 300 tcgacgacac tgcagagacc tacttcacta acaaccggta cagttcgtgg accagatggg 360 tgaggtggag tacgcgcccg gggagcccaa gggcacgccc tggcacccgc accgcggctt 420 cgagaccgtc acgaataact tcgtatagca tacattatac gaagttataa gcttgcatgc 480 ctgcaggtcg gccgccacga ccggccggcc ggtgccgcca ccatcccctg acccacgccc 540 ctgacccctc acaaggagac gaccttccat gaccgagtac aagcccacgg tgcgcctcgc 600 cacccgcgac gacgtccccc gggccgtacg caccctcgcc gccgcgttcg ccgactaccc 660 cgccacgcgc cacaccgtcg acccggaccg ccacatcgag cgggtcaccg agctgcaaga 720 actcttcctc acgcgcgtcg ggctcgacat cggcaaggtg tgggtcgcgg acgacggcgc 780 cgcggtggcg gtctggacca cgccggagag cgtcgaagcg ggggcggtgt tcgccgagat 840 cggcccgcgc atggccgagt tgagcggttc ccggctggcc gcgcagcaac agatggaagg 900 cctcctggcg ccgcaccggc ccaaggagcc cgcgtggttc ctggccaccg tcggcgtctc 960 gcccgaccac cagggcaagg gtctgggcag cgccgtcgtg ctccccggag tggaggcggc 1020 cgagcgcgcc ggggtgcccg ccttcctgga gacctccgcg ccccgcaacc tccccttcta 1080 cgagcggctc ggcttcaccg tcaccgccga cgtcgagtgc ccgaaggacc gcgcgacctg 1140 gtgcatgacc cgcaagcccg gtgcctgacg cccgccccac gacccgcagc gcccgaccga 1200 aaggagcgca cgaccccatg gctccgaccg aagccgaccc gggcggcccc gccgaccccg 1260 cacccgcccc cgaggcccac cgactctaga ggatcataat cagccatacc acatttgtag 1320 aggttttact tgctttaaaa aacctcccac acctccccct gaacctgaaa cataaaatga 1380 atgcaattgt tgttgttaac ttgtttattg cagcttataa tggttacaaa taaagcaata 1440 gcatcacaaa tttcacaaat aaagcatttt tttcactgca ttctagttgt ggtttgtcca 1500 aactcatcaa tgtatcttat catgtctgga tccgtgtcat gtcggcgacc ctacgccccc 1560 aactgagaga actcaaaggt taccccagtt ggggcactac tcccgaaaac cgcttctgga 1620 tccataactt cgtatagcat acattatacg aagttatacc gggccaccat ggtcgcgagt 1680 agcttggcac tggccgtcgt tttacaacgt cgtgactggg aaaaccctgg cgttacccaa 1740 cttaatcgcc ttgcagcaca tccccctttc gccagctggc gtaatagcga agaggcccgc 1800 accgatcgcc cttcccaaca gttgcgcagc ctgaatggcg aatggcgctt tgcctggttt 1860 ccggcaccag aagcggtgcc ggaaagctgg ctggagtgcg atcttcctga ggccgatact 1920 gtcgtcgtcc cctcaaactg gcagatgcac ggttacgatg cgcccatcta caccaacgta 1980 acctatccca ttacggtcaa tccgccgttt gttcccacgg agaatccgac gggttgttac 2040 tcgctcacat ttaatgttga tgaaagctgg ctacaggaag gccagacgcg aattattttt 2100 gatggcgtta actcggcgtt tcatctgtgg tgcaacgggc gctgggtcgg ttacggccag 2160 gacagtcgtt tgccgtctga atttgacctg agcgcatttt tacgcgccgg agaaaaccgc 2220 ctcgcggtga tggtgctgcg ttggagtgac ggcagttatc tggaagatca ggatatgtgg 2280 cggatgagcg gcattttccg tgacgtctcg ttgctgcata aaccgactac acaaatcagc 2340 gatttccatg ttgccactcg ctttaatgat gatttcagcc gcgctgtact ggaggctgaa 2400 gttcagatgt gcggcgagtt gcgtgactac ctacgggtaa cagtttcttt atggcagggt 2460 gaaacgcagg tcgccagcgg caccgcgcct ttcggcggtg aaattatcga tgagcgtggt 2520 ggttatgccg atcgcgtcac actacgtctg aacgtcgaaa acccgaaact gtggagcgcc 2580 gaaatcccga atctctatcg tgcggtggtt gaactgcaca ccgccgacgg cacgctgatt 2640 gaagcagaag cctgcgatgt cggtttccgc gaggtgcgga ttgaaaatgg tctgctgctg 2700 ctgaacggca agccgttgct gattcgaggc gttaaccgtc acgagcatca tcctctgcat 2760 ggtcaggtca tggatgagca gacgatggtg caggatatcc tgctgatgaa gcagaacaac 2820 tttaacgccg tgcgctgttc gcattatccg aaccatccgc tgtggtacac gctgtgcgac 2880 cgctacggcc tgtatgtggt ggatgaagcc aatattgaaa cccacggcat ggtgccaatg 2940 aatcgtctga ccgatgatcc gcgctggcta ccggcgatga gcgaacgcgt aacgcgaatg 3000 gtgcagcgcg atcgtaatca cccgagtgtg atcatctggt cgctggggaa tgaatcaggc 3060 cacggcgcta atcacgacgc gctgtatcgc tggatcaaat ctgtcgatcc ttcccgcccg 3120 gtgcagtatg aaggcggcgg agccgacacc acggccaccg atattatttg cccgatgtac 3180 gcgcgcgtgg atgaagacca gcccttcccg gctgtgccga aatggtccat caaaaaatgg 3240 ctttcgctac ctggagagac gcgcccgctg atcctttgcg aatacgccca cgcgatgggt 3300 aacagtcttg gcggtttcgc taaatactgg caggcgtttc gtcagtatcc ccgtttacag 3360 ggcggcttcg tctgggactg ggtggatcag tcgctgatta aatatgatga aaacggcaac 3420 ccgtggtcgg cttacggcgg tgattttggc gatacgccga acgatcgcca gttctgtatg 3480 aacggtctgg tctttgccga ccgcacgccg catccagcgc tgacggaagc aaaacaccag 3540 cagcagtttt tccagttccg tttatccggg caaaccatcg aagtgaccag cgaatacctg 3600 ttccgtcata gcgataacga gctcctgcac tggatggtgg cgctggatgg taagccgctg 3660 gcaagcggtg aagtgcctct ggatgtcgct ccacaaggta aacagttgat tgaactgcct 3720 gaactaccgc agccggagag cgccgggcaa ctctggctca cagtacgcgt agtgcaaccg 3780 aacgcgaccg catggtcaga agccgggcac atcagcgcct ggcagcagtg gcgtctggcg 3840 gaaaacctca gtgtgacgct ccccgccgcg tcccacgcca tcccgcatct gaccaccagc 3900 gaaatggatt tttgcatcga gctgggtaat aagcgttggc aatttaaccg ccagtcaggc 3960 tttctttcac agatgtggat tggcgataaa aaacaactgc tgacgccgct gcgcgatcag 4020 ttcacccgtg caccgctgga taacgacatt ggcgtaagtg aagcgacccg cattgaccct 4080 aacgcctggg tcgaacgctg gaaggcggcg ggccattacc aggccgaagc agcgttgttg 4140 cagtgcacgg cagatacact tgctgatgcg gtgctgatta cgaccgctca cgcgtggcag 4200 catcagggga aaaccttatt tatcagccgg aaaacctacc ggattgatgg tagtggtcaa 4260 atggcgatta ccgttgatgt tgaagtggcg agcgatacac cgcatccggc gcggattggc 4320 ctgaactgcc agctggcgca ggtagcagag cgggtaaact ggctcggatt agggccgcaa 4380 gaaaactatc ccgaccgcct tactgccgcc tgttttgacc gctgggatct gccattgtca 4440 gacatgtata ccccgtacgt cttcccgagc gaaaacggtc tgcgctgcgg gacgcgcgaa 4500 ttgaattatg gcccacacca gtggcgcggc gacttccagt tcaacatcag ccgctacagt 4560 caacagcaac tgatggaaac cagccatcgc catctgctgc acgcggaaga aggcacatgg 4620 ctgaatatcg acggtttcca tatggggatt ggtggcgacg actcctggag cccgtcagta 4680 tcggcggaat tccagctgag cgccggtcgc taccattacc agttggtctg gtgtcaaaaa 4740 taataataac cgggcagggg ggatctttgt gaaggaacct tacttctgtg gtgtgacata 4800 attggacaaa ctacctacag agatttaaag ctctaaggta aatataaaat ttttaagtgt 4860 ataatgtgtt aaactactga ttctaattgt ttgtgtattt tagattccaa cctatggaac 4920 tgatgaatgg gagcagtggt ggaatgccag atccagacat gataagatac attgatgagt 4980 ttggacaaac cacaactaga atgcagtgaa aaaaatgctt tatttgtgaa atttgtgatg 5040 ctattgcttt atttgtaacc attataagct gcaataaaca agttaacaac aacaattgca 5100 ttcattttat gtttcaggtt cagggggagg tgtgggaggt tttttaaagc aagtaaaacc 5160 tctacaaatg tggtatggct gattatgatc tgcggccgca gggcctcgtg atacgcctat 5220 ttttataggt taatgtcatg ataataatgg tttcttagac gtcaggtggc acttttcggg 5280 gaaatgtgcg cggaacccct atttgtttat ttttctaaat acattcaaat atgtatccgc 5340 tcatgagaca ataaccctga taaatgcttc aataatattg aaaaaggaag agtatgagta 5400 ttcaacattt ccgtgtcgcc cttattccct tttttgcggc attttgcctt cctgtttttg 5460 ctcacccaga aacgctggtg aaagtaaaag atgctgaaga tcagttgggt gcacgagtgg 5520 gttacatcga actggatctc aacagcggta agatccttga gagttttcgc cccgaagaac 5580 gttttccaat gatgagcact tttaaagttc tgctatgtgg cgcggtatta tcccgtattg 5640 acgccgggca agagcaactc ggtcgccgca tacactattc tcagaatgac ttggttgagt 5700 actcaccagt cacagaaaag catcttacgg atggcatgac agtaagagaa ttatgcagtg 5760 ctgccataac catgagtgat aacactgcgg ccaacttact tctgacaacg atcggaggac 5820 cgaaggagct aaccgctttt ttgcacaaca tgggggatca tgtaactcgc cttgatcgtt 5880 gggaaccgga gctgaatgaa gccataccaa acgacgagcg tgacaccacg atgcctgtag 5940 caatggcaac aacgttgcgc aaactattaa ctggcgaact acttactcta gcttcccggc 6000 aacaattaat agactggatg gaggcggata aagttgcagg accacttctg cgctcggccc 6060 ttccggctgg ctggtttatt gctgataaat ctggagccgg tgagcgtggg tctcgcggta 6120 tcattgcagc actggggcca gatggtaagc cctcccgtat cgtagttatc tacacgacgg 6180 ggagtcaggc aactatggat gaacgaaata gacagatcgc tgagataggt gcctcactga 6240 ttaagcattg gtaactgtca gaccaagttt actcatatat actttagatt gatttaaaac 6300 ttcattttta atttaaaagg atctaggtga agatcctttt tgataatctc atgaccaaaa 6360 tcccttaacg tgagttttcg ttccactgag cgtcagaccc cgtagaaaag atcaaaggat 6420 cttcttgaga tccttttttt ctgcgcgtaa tctgctgctt gcaaacaaaa aaaccaccgc 6480 taccagcggt ggtttgtttg ccggatcaag agctaccaac tctttttccg aaggtaactg 6540 gcttcagcag agcgcagata ccaaatactg tccttctagt gtagccgtag ttaggccacc 6600 acttcaagaa ctctgtagca ccgcctacat acctcgctct gctaatcctg ttaccagtgg 6660 ctgctgccag tggcgataag tcgtgtctta ccgggttgga ctcaagacga tagttaccgg 6720 ataaggcgca gcggtcgggc tgaacggggg gttcgtgcac acagcccagc ttggagcgaa 6780 cgacctacac cgaactgaga tacctacagc gtgagctatg agaaagcgcc acgcttcccg 6840 aagggagaaa ggcggacagg tatccggtaa gcggcagggt cggaacagga gagcgcacga 6900 gggagcttcc agggggaaac gcctggtatc tttatagtcc tgtcgggttt cgccacctct 6960 gacttgagcg tcgatttttg tgatgctcgt caggggggcg gagcctatgg aaaaacgcca 7020 gcaacgcggc ctttttacgg ttcctggcct tttgctggcc ttttgctcac atgttctttc 7080 ctgcgttatc ccctgattct gtggataacc gtattaccgc ctttgagtga gctgataccg 7140 ctcgccgcag ccgaacgacc gagcgcagcg agtcagtgag cgaggaagcg gaagagcgcc 7200 caatacgcaa accgcctctc cccgcgcgtt ggccgattca ttaatgcagc tggcacgaca 7260 ggtttcccga ctggaaagcg ggcagtgagc gcaacgcaat taatgtgagt tagctcactc 7320 attaggcacc ccaggcttta cactttatgc ttccggctcg tatgttgtgt ggaattgtga 7380 gcggataaca atttcacaca ggaaacagct atgaccatga ttacgccaag ctggcgcg 7438 12 12538 DNA pROSA-SA-C31-Int(CNLS) 12 tttgagtgag ctgataccgc tcgccgcagc cgaacgaccg agcgcagcga gtcagtgagc 60 gaggaagcgg aagagcgccc aatacgcaaa ccgcctctcc ccgcgcgttg gccgattcat 120 taatgcagct ggcacgacag gtttcccgac tggaaagcgg gcagtgagcg caacgcaatt 180 aatgtgagtt agctcactca ttaggcaccc caggctttac actttatgct tccggctcgt 240 atgttgtgtg gaattgtgag cggataacaa tttcacacag gaaacagcta tgaccatgat 300 tacgccaagc gcgcaattaa ccctcactaa agggaacaaa agctgtcgag atctagatat 360 cgatggccat agagttacgc tagggataac agggtaatat agccgcggca ggccctccga 420 gcgtggtgga gccgttctgt gagacagccg ggtacgagtc gtgacgctgg aaggggcaag 480 cgggtggtgg gcaggaatgc ggtccgccct gcagcaaccg gagggggagg gagaagggag 540 cggaaaagtc tccaccggac gcggccatgg ctcggggggg ggggggcagc ggaggagcgc 600 ttccggccga cgtctcgtcg ctgattggct tcttttcctc ccgccgtgtg tgaaaacaca 660 aatggcgtgt tttggttggc gtaaggcgcc tgtcagttaa cggcagccgg agtgcgcagc 720 cgccggcagc ctcgctctgc ccactgggtg gggcgggagg taggtggggt gaggcgagct 780 ggacgtgcgg gcgcggtcgg cctctggcgg ggcgggggag gggagggagg gtcagcgaaa 840 gtagctcgcg cgcgagcggc cgcccaccct ccccttcctc tgggggagtc gttttacccg 900 ccgccggccg ggcctcgtcg tctgattggc tctcggggcc cagaaaactg gcccttgcca 960 ttggctcgtg ttcgtgcaag ttgagtccat ccgccggcca gcgggggcgg cgaggaggcg 1020 ctcccaggtt ccggccctcc cctcggcccc gcgccgcaga gtctggccgc gcgcccctgc 1080 gcaacgtggc aggaagcgcg cgctgggggc ggggacgggc agtagggctg agcggctgcg 1140 gggcgggtgc aagcacgttt ccgacttgag ttgcctcaag aggggcgtgc tgagccagac 1200 ctccatcgcg cactccgggg agtggaggga aggagcgagg gctcagttgg gctgttttgg 1260 aggcaggaag cacttgctct cccaaagtcg ctctgagttg ttatcagtaa gggagctgca 1320 gtggagtagg cggggagaag gccgcaccct tctccggagg ggggagggga gtgttgcaat 1380 acctttctgg gagttctctg ctgcctcctg gcttctgagg accgccctgg gcctgggaga 1440 atcccttccc cctcttccct cgtgatctgc aactccagtc tttctaggta accgatatcc 1500 ctgcaggggt gacctgcacg tctagggcgc agtagtccag ggtttccttg atgatgtcat 1560 acttatcctg tccctttttt ttccacagct cgcggttgag gacaaactct tcgcggtctt 1620 tccagtactc ctgcaggtga ctgactgagt cgacttaatt aaggccatag cggccatttg 1680 gccgcccgat atgacacaag gggttgtgac cggggtggac acgtacgcgg gtgcttacga 1740 ccgtcagtcg cgcgagcgcg agaattcgag cgcagcaagc ccagcgacac agcgtagcgc 1800 caacgaagac aaggcggccg accttcagcg cgaagtcgag cgcgacgggg gccggttcag 1860 gttcgtcggg catttcagcg aagcgccggg cacgtcggcg ttcgggacgg cggagcgccc 1920 ggagttcgaa cgcatcctga acgaatgccg cgccgggcgg ctcaacatga tcattgtcta 1980 tgacgtgtcg cgcttctcgc gcctgaaggt catggacgcg attccgattg tctcggaatt 2040 gctcgccctg ggcgtgacga ttgtttccac tcaggaaggc gtcttccggc agggaaacgt 2100 catggacctg attcacctga ttatgcggct cgacgcgtcg cacaaagaat cttcgctgaa 2160 gtcggcgaag attctcgaca cgaagaacct tcagcgcgaa ttgggcgggt acgtcggcgg 2220 gaaggcgcct tacggcttcg agcttgtttc ggagacgaag gagatcacgc gcaacggccg 2280 aatggtcaat gtcgtcatca acaagcttgc gcactcgacc actcccctta ccggaccctt 2340 cgagttcgag cccgacgtaa tccggtggtg gtggcgtgag atcaagacgc acaaacacct 2400 tcccttcaag ccgggcagtc aagccgccat tcacccgggc agcatcacgg ggctttgtaa 2460 gcgcatggac gctgacgccg tgccgacccg gggcgagacg attgggaaga agaccgcttc 2520 aagcgcctgg gacccggcaa ccgttatgcg aatccttcgg gacccgcgta ttgcgggctt 2580 cgccgctgag gtgatctaca agaagaagcc ggacggcacg ccgaccacga agattgaggg 2640 ttaccgcatt cagcgcgacc cgatcacgct ccggccggtc gagcttgatt gcggaccgat 2700 catcgagccc gctgagtggt atgagcttca ggcgtggttg gacggcaggg ggcgcggcaa 2760 ggggctttcc cgggggcaag ccattctgtc cgccatggac aagctgtact gcgagtgtgg 2820 cgccgtcatg acttcgaagc gcggggaaga atcgatcaag gactcttacc gctgccgtcg 2880 ccggaaggtg gtcgacccgt ccgcacctgg gcagcacgaa ggcacgtgca acgtcagcat 2940 ggcggcactc gacaagttcg ttgcggaacg catcttcaac aagatcaggc acgccgaagg 3000 cgacgaagag acgttggcgc ttctgtggga agccgcccga cgcttcggca agctcactga 3060 ggcgcctgag aagagcggcg aacgggcgaa ccttgttgcg gagcgcgccg acgccctgaa 3120 cgcccttgaa gagctgtacg aagaccgcgc ggcaggcgcg tacgacggac ccgttggcag 3180 gaagcacttc cggaagcaac aggcagcgct gacgctccgg cagcaagggg cggaagagcg 3240 gcttgccgaa cttgaagccg ccgaagcccc gaagcttccc cttgaccaat ggttccccga 3300 agacgccgac gctgacccga ccggccctaa gtcgtggtgg gggcgcgcgt cagtagacga 3360 caagcgcgtg ttcgtcgggc tcttcgtaga caagatcgtt gtcacgaagt cgactacggg 3420 cagggggcag ggaacgccca tcgagaagcg cgcttcgatc acgtgggcga agccgccgac 3480 cgacgacgac gaagacgacg cccaggacgg cacggaagac gtagcggcgc ctaagaagaa 3540 gaggaaggtt tagactctcg agatccaggc gcggatcaat aaaagatcat tattttcaat 3600 agatctgtgt gttggttttt tgtgtgcctt gggggagggg gaggccagaa tgaggcgcgg 3660 ccaaggggga gggggaggcc agaatgacct tgggggaggg ggaggccaga atgaccttgg 3720 gggaggggga ggccagaatg aggcgcgccg gtaaccgaag ttcctatact ttctagagaa 3780 taggaacttc ggaataggaa cttcttaggt caattctacc gggtagggga ggcgcttttc 3840 ccaaggcagt ctggagcatg cgctttagca gccccgctgg gcacttggcg ctacacaagt 3900 ggcctctggc ctcgcacaca ttccacatcc accggtaggc gccaaccggc tccgttcttt 3960 ggtggcccct tcgcgccacc ttctactcct cccctagtca ggaagttccc ccccgccccg 4020 cagctcgcgt cgtgcaggac gtgacaaatg gaagtagcac gtctcactag tctcgtgcag 4080 atggacagca ccgctgagca atggaagcgg gtaggccttt ggggcagcgg ccaatagcag 4140 ctttgctcct tcgctttctg ggctcagagg ctgggaaggg gtgggtccgg gggcgggctc 4200 aggggcgggc tcaggggcgg ggcgggcgcc cgaaggtcct ccggaggccc ggcattctgc 4260 acgcttcaaa agcgcacgtc tgccgcgctg ttctcctctt cctcatctcc gggcctttcg 4320 acctgcagcc aatatgggat cggccattga acaagatgga ttgcacgcag gttctccggc 4380 cgcttgggtg gagaggctat tcggctatga ctgggcacaa cagacaatcg gctgctctga 4440 tgccgccgtg ttccggctgt cagcgcaggg gcgcccggtt ctttttgtca agaccgacct 4500 gtccggtgcc ctgaatgaac tgcaggacga ggcagcgcgg ctatcgtggc tggccacgac 4560 gggcgttcct tgcgcagctg tgctcgacgt tgtcactgaa gcgggaaggg actggctgct 4620 attgggcgaa gtgccggggc aggatctcct gtcatctcac cttgctcctg ccgagaaagt 4680 atccatcatg gctgatgcaa tgcggcggct gcatacgctt gatccggcta cctgcccatt 4740 cgaccaccaa gcgaaacatc gcatcgagcg agcacgtact cggatggaag ccggtcttgt 4800 cgatcaggat gatctggacg aagagcatca ggggctcgcg ccagccgaac tgttcgccag 4860 gctcaaggcg cgcatgcccg acggcgagga tctcgtcgtg acccatggcg atgcctgctt 4920 gccgaatatc atggtggaaa atggccgctt ttctggattc atcgactgtg gccggctggg 4980 tgtggcggac cgctatcagg acatagcgtt ggctacccgt gatattgctg aagagcttgg 5040 cggcgaatgg gctgaccgct tcctcgtgct ttacggtatc gccgctcccg attcgcagcg 5100 catcgccttc tatcgccttc ttgacgagtt cttctgaggg gatcgatccg ctgtaagtct 5160 gcagaaattg atgatctatt aaacaataaa gatgtccact aaaatggaag tttttcctgt 5220 catactttgt taagaagggt gagaacagag tacctacatt ttgaatggaa ggattggagc 5280 tacgggggtg ggggtggggt gggattagat aaatgcctgc tctttactga aggctcttta 5340 ctattgcttt atgataatgt ttcatagttg gatatcataa tttaaacaag caaaaccaaa 5400 ttaagggcca gctcattcct cccactcatg atctatagat ctatagatct ctcgtgggat 5460 cattgttttt ctcttgattc ccactttgtg gttctaagta ctgtggtttc caaatgtgtc 5520 agtttcatag cctgaagaac gagatcagca gcctctgttc cacatacact tcattctcag 5580 tattgttttg ccaagttcta attccatcag aagctgactc tagatcccgc gccgaagttc 5640 ctatactttc tagagaatag gaacttcgga ataggaactt caagcttaag cgctagaaga 5700 tgggcgggag tcttctgggc aggcttaaag gctaacctgg tgtgtgggcg ttgtcctgca 5760 ggggaattga acaggtgtaa aattggaggg acaagacttc ccacagattt tcggttttgt 5820 cgggaagttt tttaataggg gcaaataagg aaaatgggag gataggtagt catctggggt 5880 tttatgcagc aaaactacag gttattattg cttgtgatcc gcctcggagt attttccatc 5940 gaggtagatt aaagacatgc tcacccgagt tttatactct cctgcttgag atccttacta 6000 cagtatgaaa ttacagtgtc gcgagttaga ctatgtaagc agaattttaa tcatttttaa 6060 agagcccagt acttcatatc catttctccc gctccttctg cagccttatc aaaaggtatt 6120 ttagaacact cattttagcc ccattttcat ttattatact ggcttatcca acccctagac 6180 agagcattgg cattttccct ttcctgatct tagaagtctg atgactcatg aaaccagaca 6240 gattagttac atacaccaca aatcgaggct gtagctgggg cctcaacact gcagttcttt 6300 tataactcct tagtacactt tttgttgatc ctttgccttg atccttaatt ttcagtgtct 6360 atcacctctc ccgtcagtgg tgttccacat ttgggcctat tctcagtcca gggagtttta 6420 caacaataga tgtattgaga atccaaccta aagcttaact ttccactccc atgaatgcct 6480 ctctcctttt tctccattta taaactgagc tattaaccat taatggttcc aggtggatgt 6540 ctcctcccca tattacctga tgtatcttac atattgccag gctgatattt taagacatta 6600 aaaggtatat ttcattattg agccacatgg tattgattac tgcttactaa aattttgtca 6660 ttgtacacat ctgtaaaagg tggttccttt tggaatgcaa agttcaggtg tttgttgtct 6720 ttcctgacct aaggtcttgt gagcttgtat tttttctatt taagcagtgc tttctcttgg 6780 actggcttga ctcatggcat tctacacgtt attgctggtc taaatgtgat tttgccaagc 6840 ttcttcagga cctataattt tgcttgactt gtagccaaac acaagtaaaa tgattaagca 6900 acaaatgtat ttgtgaagct tggtttttag gttgttgtgt tgtgtgtgct tgtgctctat 6960 aataatacta tccaggggct ggagaggtgg ctcggagttc aagagcacag actgctcttc 7020 cagaagtcct gagttcaatt cccagcaacc acatggtggc tcacaaccat ctgtaatggg 7080 atctgatgcc ctcttctggt gtgtctgaag accacaagtg tattcacatt aaataaataa 7140 atcctccttc ttcttctttt tttttttttt aaagagaata ctgtctccag tagaatttac 7200 tgaagtaatg aaatactttg tgtttgttcc aatatggtag ccaataatca aattactctt 7260 taagcactgg aaatgttacc aaggaactaa tttttatttg aagtgtaact gtggacagag 7320 gagccataac tgcagacttg tgggatacag aagaccaatg cagactttaa tgtcttttct 7380 cttacactaa gcaataaaga aataaaaatt gaacttctag tatcctattt gtttaaactg 7440 ctagctttac ttaacttttg tgcttcatct atacaaagct gaaagctaag tctgcagcca 7500 ttactaaaca tgaaagcaag taatgataat tttggatttc aaaaatgtag ggccagagtt 7560 tagccagcca gtggtggtgc ttgcctttat gcctttaatc ccagcactct ggaggcagag 7620 acaggcagat ctctgagttt gagcccagcc tggtctacac atcaagttct atctaggata 7680 gccaggaata cacacagaaa ccctgttggg gaggggggct ctgagatttc ataaaattat 7740 aattgaagca ttccctaatg agccactatg gatgtggcta aatccgtcta cctttctgat 7800 gagatttggg tattattttt tctgtctctg ctgttggttg ggtcttttga cactgtgggc 7860 tttctttaaa gcctccttcc tgccatgtgg tctcttgttt gctactaact tcccatggct 7920 taaatggcat ggctttttgc cttctaaggg cagctgctga gatttgcagc ctgatttcca 7980 gggtggggtt gggaaatctt tcaaacacta aaattgtcct ttaatttttt ttttaaaaaa 8040 tgggttatat aataaacctc ataaaatagt tatgaggagt gaggtggact aatattaaat 8100 gagtccctcc cctataaaag agctattaag gctttttgtc ttatacttaa cttttttttt 8160 aaatgtggta tctttagaac caagggtctt agagttttag tatacagaaa ctgttgcatc 8220 gcttaatcag attttctagt ttcaaatcca gagaatccaa attcttcaca gccaaagtca 8280 aattaagaat ttctgacttt taatgttaat ttgcttactg tgaatataaa aatgatagct 8340 tttcctgagg cagggtctca ctatgtatct ctgcctgatc tgcaacaaga tatgtagact 8400 aaagttctgc ctgcttttgt ctcctgaata ctaaggttaa aatgtagtaa tacttttgga 8460 acttgcaggt cagattcttt tataggggac acactaaggg agcttgggtg atagttggta 8520 aaatgtgttt caagtgatga aaacttgaat tattatcacc gcaacctact ttttaaaaaa 8580 aaaagccagg cctgttagag catgcttaag ggatccctag gacttgctga gcacacaaga 8640 gtagttactt ggcaggctcc tggtgagagc atatttcaaa aaacaaggca gacaaccaag 8700 aaactacagt taaggttacc tgtctttaaa ccatctgcat atacacaggg atattaaaat 8760 attccaaata atatttcatt caagttttcc cccatcaaat tgggacatgg atttctccgg 8820 tgaataggca gagttggaaa ctaaacaaat gttggttttg tgatttgtga aattgttttc 8880 aagtgatagt taaagcccat gagatacaga acaaagctgc tatttcgagg tctcttggtt 8940 tatactcaga agcacttctt tgggtttccc tgcactatcc tgatcatgtg ctaggcctac 9000 cttaggctga ttgttgttca aataaactta agtttcctgt caggtgatgt catatgattt 9060 catatatcaa ggcaaaacat gttatatatg ttaaacattt gtacttaatg tgaaagttag 9120 gtctttgtgg gtttgatttt taattttcaa aacctgagct aaataagtca tttttacatg 9180 tcttacattt ggtggaattg tataattgtg gtttgcaggc aagactctct gacctagtaa 9240 ccctacctat agagcacttt gctgggtcac aagtctagga gtcaagcatt tcaccttgaa 9300 gttgagacgt tttgttagtg tatactagtt tatatgttgg aggacatgtt tatccagaag 9360 atattcagga ctatttttga ctgggctaag gaattgattc tgattagcac tgttagtgag 9420 cattgagtgg cctttaggct tgaattggag tcacttgtat atctcaaata atgctggcct 9480 tttttaaaaa gcccttgttc tttatcaccc tgttttctac ataatttttg ttcaaagaaa 9540 tacttgtttg gatctccttt tgacaacaat agcatgtttt caagccatat tttttttcct 9600 tttttttttt ttttttggtt tttcgagaca gggtttctct gtatagccct ggctgtcctg 9660 gaactcactt tgtagaccag gctggcctcg aactcagaaa tccgcctgcc tctgcctcct 9720 gagtgccggg attaaaggcg tgcaccacca cgcctggcta agttggatat tttgttatat 9780 aactataacc aatactaact ccactgggtg gatttttaat tcagtcagta gtcttaagtg 9840 gtctttattg gcccttcatt aaaatctact gttcactcta acagaggctg ttggtactag 9900 tggcacttaa gcaacttcct acggatatac tagcagatta agggtcaggg atagaaacta 9960 gtctagcgtt ttgtatacct accagcttta tactaccttg ttctgataga aatatttcag 10020 gacatctagc acccaattcg ccctatagtg agtcgtatta caattcactg gccgtcgttt 10080 tacaacgtcg tgactgggaa aaccctggcg ttacccaact taatcgcctt gcagcacatc 10140 cccctttcgc cagctggcgt aatagcgaag aggcccgcac cgatcgccct tcccaacagt 10200 tgcgcagcct gaatggcgaa tgggacgcgc cctgtagcgg cgcattaagc gcggcgggtg 10260 tggtggttac gcgcagcgtg accgctacac ttgccagcgc cctagcgccc gctcctttcg 10320 ctttcttccc ttcctttctc gccacgttcg ccggctttcc ccgtcaagct ctaaatcggg 10380 ggctcccttt agggttccga tttagtgctt tacggcacct cgaccccaaa aaacttgatt 10440 agggtgatgg ttcacgtagt gggccatcgc cctgatagac ggtttttcgc cctttgacgt 10500 tggagtccac gttctttaat agtggactct tgttccaaac tggaacaaca ctcaacccta 10560 tctcggtcta ttcttttgat ttataaggga ttttgccgat ttcggcctat tggttaaaaa 10620 atgagctgat ttaacaaaaa tttaacgcga attttaacaa aatattaacg cttacaattt 10680 aggtggcact tttcggggaa atgtgcgcgg aacccctatt tgtttatttt tctaaataca 10740 ttcaaatatg tatccgctca tgagacaata accctgataa atgcttcaat aatattgaaa 10800 aaggaagagt atgagtattc aacatttccg tgtcgccctt attccctttt ttgcggcatt 10860 ttgccttcct gtttttgctc acccagaaac gctggtgaaa gtaaaagatg ctgaagatca 10920 gttgggtgca cgagtgggtt acatcgaact ggatctcaac agcggtaaga tccttgagag 10980 ttttcgcccc gaagaacgtt ttccaatgat gagcactttt aaagttctgc tatgtggcgc 11040 ggtattatcc cgtattgacg ccgggcaaga gcaactcggt cgccgcatac actattctca 11100 gaatgacttg gttgagtact caccagtcac agaaaagcat cttacggatg gcatgacagt 11160 aagagaatta tgcagtgctg ccataaccat gagtgataac actgcggcca acttacttct 11220 gacaacgatc ggaggaccga aggagctaac cgcttttttg cacaacatgg gggatcatgt 11280 aactcgcctt gatcgttggg aaccggagct gaatgaagcc ataccaaacg acgagcgtga 11340 caccacgatg cctgtagcaa tggcaacaac gttgcgcaaa ctattaactg gcgaactact 11400 tactctagct tcccggcaac aattaataga ctggatggag gcggataaag ttgcaggacc 11460 acttctgcgc tcggcccttc cggctggctg gtttattgct gataaatctg gagccggtga 11520 gcgtgggtct cgcggtatca ttgcagcact ggggccagat ggtaagccct cccgtatcgt 11580 agttatctac acgacgggga gtcaggcaac tatggatgaa cgaaatagac agatcgctga 11640 gataggtgcc tcactgatta agcattggta actgtcagac caagtttact catatatact 11700 ttagattgat ttaaaacttc atttttaatt taaaaggatc taggtgaaga tcctttttga 11760 taatctcatg accaaaatcc cttaacgtga gttttcgttc cactgagcgt cagaccccgt 11820 agaaaagatc aaaggatctt cttgagatcc tttttttctg cgcgtaatct gctgcttgca 11880 aacaaaaaaa ccaccgctac cagcggtggt ttgtttgccg gatcaagagc taccaactct 11940 ttttccgaag gtaactggct tcagcagagc gcagatacca aatactgtcc ttctagtgta 12000 gccgtagtta ggccaccact tcaagaactc tgtagcaccg cctacatacc tcgctctgct 12060 aatcctgtta ccagtggctg ctgccagtgg cgataagtcg tgtcttaccg ggttggactc 12120 aagacgatag ttaccggata aggcgcagcg gtcgggctga acggggggtt cgtgcacaca 12180 gcccagcttg gagcgaacga cctacaccga actgagatac ctacagcgtg agctatgaga 12240 aagcgccacg cttcccgaag ggagaaaggc ggacaggtat ccggtaagcg gcagggtcgg 12300 aacaggagag cgcacgaggg agcttccagg gggaaacgcc tggtatcttt atagtcctgt 12360 cgggtttcgc cacctctgac ttgagcgtcg atttttgtga tgctcgtcag gggggcggag 12420 cctatggaaa aacgccagca acgcggcctt tttacggttc ctggcctttt gctggccttt 12480 tgctcacatg ttctttcctg cgttatcccc tgattctgtg gataaccgta ttaccgcc 12538 13 12645 DNA pROSA-SA-C31-Int(CNLS)-CO 13 tttgagtgag ctgataccgc tcgccgcagc cgaacgaccg agcgcagcga gtcagtgagc 60 gaggaagcgg aagagcgccc aatacgcaaa ccgcctctcc ccgcgcgttg gccgattcat 120 taatgcagct ggcacgacag gtttcccgac tggaaagcgg gcagtgagcg caacgcaatt 180 aatgtgagtt agctcactca ttaggcaccc caggctttac actttatgct tccggctcgt 240 atgttgtgtg gaattgtgag cggataacaa tttcacacag gaaacagcta tgaccatgat 300 tacgccaagc gcgcaattaa ccctcactaa agggaacaaa agctgtcgag atctagatat 360 cgatggccat agagttacgc tagggataac agggtaatat agccgcggca ggccctccga 420 gcgtggtgga gccgttctgt gagacagccg ggtacgagtc gtgacgctgg aaggggcaag 480 cgggtggtgg gcaggaatgc ggtccgccct gcagcaaccg gagggggagg gagaagggag 540 cggaaaagtc tccaccggac gcggccatgg ctcggggggg ggggggcagc ggaggagcgc 600 ttccggccga cgtctcgtcg ctgattggct tcttttcctc ccgccgtgtg tgaaaacaca 660 aatggcgtgt tttggttggc gtaaggcgcc tgtcagttaa cggcagccgg agtgcgcagc 720 cgccggcagc ctcgctctgc ccactgggtg gggcgggagg taggtggggt gaggcgagct 780 ggacgtgcgg gcgcggtcgg cctctggcgg ggcgggggag gggagggagg gtcagcgaaa 840 gtagctcgcg cgcgagcggc cgcccaccct ccccttcctc tgggggagtc gttttacccg 900 ccgccggccg ggcctcgtcg tctgattggc tctcggggcc cagaaaactg gcccttgcca 960 ttggctcgtg ttcgtgcaag ttgagtccat ccgccggcca gcgggggcgg cgaggaggcg 1020 ctcccaggtt ccggccctcc cctcggcccc gcgccgcaga gtctggccgc gcgcccctgc 1080 gcaacgtggc aggaagcgcg cgctgggggc ggggacgggc agtagggctg agcggctgcg 1140 gggcgggtgc aagcacgttt ccgacttgag ttgcctcaag aggggcgtgc tgagccagac 1200 ctccatcgcg cactccgggg agtggaggga aggagcgagg gctcagttgg gctgttttgg 1260 aggcaggaag cacttgctct cccaaagtcg ctctgagttg ttatcagtaa gggagctgca 1320 gtggagtagg cggggagaag gccgcaccct tctccggagg ggggagggga gtgttgcaat 1380 acctttctgg gagttctctg ctgcctcctg gcttctgagg accgccctgg gcctgggaga 1440 atcccttccc cctcttccct cgtgatctgc aactccagtc tttctaggta accgatatcc 1500 ctgcaggggt gacctgcacg tctagggcgc agtagtccag ggtttccttg atgatgtcat 1560 acttatcctg tccctttttt ttccacagct cgcggttgag gacaaactct tcgcggtctt 1620 tccagtactc ctgcaggtga ctgactgagt cgacttaatt aaggccatag cggccattta 1680 aatagttacg ctagggataa cagggtaata tagttaatta atctagaact agtggatccc 1740 ccgggctgca ggaattcgat atcgccacca tgacccaggg cgtggtgacc ggcgtggaca 1800 cctacgccgg agcctacgac aggcagagca gggagaggga gaacagctcc gccgccagcc 1860 ccgccaccca gagatccgcc aacgaggaca aggccgccga cctgcagagg gaggtggaga 1920 gggacggcgg caggttcagg ttcgtgggcc acttcagcga ggcccccggc acctccgcct 1980 tcggcaccgc cgagaggccc gagttcgaga ggatcctgaa cgagtgcagg gccggcaggc 2040 tgaacatgat catcgtgtac gatgtgagca ggttcagcag gctgaaggtc atggatgcca 2100 tccccatcgt gtccgagctg ctggccctgg gcgtgaccat cgtgagcacc caggagggcg 2160 tgttcaggca gggcaacgtg atggacctga tccacctgat catgaggctg gatgccagcc 2220 acaaggagag cagcctgaag tccgccaaga tcctggacac caagaacctg cagagagagc 2280 tgggcggcta cgtgggcggc aaggccccct acggcttcga actcgtgagc gagaccaagg 2340 agatcaccag gaacggcagg atggtgaacg tggtgatcaa caagctggcc cacagcacca 2400 cccccctgac cggccccttc gagttcgagc ccgacgtgat caggtggtgg tggagggaga 2460 tcaagaccca caagcacctg cccttcaagc ccggcagcca ggccgccatc caccccggca 2520 gcatcaccgg cctgtgcaag aggatggatg ccgatgccgt gcccaccagg ggcgagacca 2580 tcggcaagaa aaccgccagc tccgcctggg accccgccac cgtgatgagg atcctgaggg 2640 acccccggat cgccggcttc gccgccgagg tgatctacaa gaagaagccc gacggcaccc 2700 ccaccaccaa gatcgagggc tacaggatcc agagggaccc catcaccctg aggcccgtgg 2760 agctggactg cggccccatc atcgagcccg ccgagtggta cgagctgcag gcctggctgg 2820 acggcagggg caggggcaag ggcctgagca ggggccaggc catcctgtcc gccatggaca 2880 agctgtactg cgagtgcgga gccgtgatga ccagcaagag gggcgaggag agcatcaagg 2940 acagctacag atgcaggagg aggaaggtgg tggacccctc cgcccccggc cagcacgagg 3000 gcacctgcaa cgtgagcatg gccgccctgg acaagttcgt ggccgagagg atcttcaaca 3060 agatcaggca cgccgagggc gacgaggaga ccctggccct gctgtgggag gccgccagga 3120 ggttcggcaa gctgaccgag gcccccgaga agagcggcga gagggccaac ctggtggccg 3180 agagggccga tgccctgaat gccctggagg agctgtacga ggacagggcc gccggagcct 3240 acgacggccc cgtgggcagg aagcacttca ggaagcagca ggccgccctg accctgaggc 3300 agcagggagc cgaggagagg ctggccgagc tggaggccgc cgaggccccc aagctgcccc 3360 tggaccagtg gttccccgag gatgccgatg ccgaccccac cggccccaag agctggtggg 3420 gcagggccag cgtggacgac aagagggtgt tcgtgggcct gttcgtggac aagatcgtgg 3480 tgaccaagag caccaccggc aggggccagg gcacccccat cgagaagagg gccagcatca 3540 cctgggccaa gccccccacc gacgacgacg aggacgatgc ccaggacggc accgaggacg 3600 tggccgcccc caagaagaag aggaaggtgt gatgaagata tcaagcttat cgataccgtc 3660 gacctcgaga tccaggcgcg gatcaataaa agatcattat tttcaataga tctgtgtgtt 3720 ggttttttgt gtgccttggg ggagggggag gccagaatga ggcgcggcca agggggaggg 3780 ggaggccaga atgaccttgg gggaggggga ggccagaatg accttggggg agggggaggc 3840 cagaatgagg cgcgccggta accgaagttc ctatactttc tagagaatag gaacttcgga 3900 ataggaactt cttaggtcaa ttctaccggg taggggaggc gcttttccca aggcagtctg 3960 gagcatgcgc tttagcagcc ccgctgggca cttggcgcta cacaagtggc ctctggcctc 4020 gcacacattc cacatccacc ggtaggcgcc aaccggctcc gttctttggt ggccccttcg 4080 cgccaccttc tactcctccc ctagtcagga agttcccccc cgccccgcag ctcgcgtcgt 4140 gcaggacgtg acaaatggaa gtagcacgtc tcactagtct cgtgcagatg gacagcaccg 4200 ctgagcaatg gaagcgggta ggcctttggg gcagcggcca atagcagctt tgctccttcg 4260 ctttctgggc tcagaggctg ggaaggggtg ggtccggggg cgggctcagg ggcgggctca 4320 ggggcggggc gggcgcccga aggtcctccg gaggcccggc attctgcacg cttcaaaagc 4380 gcacgtctgc cgcgctgttc tcctcttcct catctccggg cctttcgacc tgcagccaat 4440 atgggatcgg ccattgaaca agatggattg cacgcaggtt ctccggccgc ttgggtggag 4500 aggctattcg gctatgactg ggcacaacag acaatcggct gctctgatgc cgccgtgttc 4560 cggctgtcag cgcaggggcg cccggttctt tttgtcaaga ccgacctgtc cggtgccctg 4620 aatgaactgc aggacgaggc agcgcggcta tcgtggctgg ccacgacggg cgttccttgc 4680 gcagctgtgc tcgacgttgt cactgaagcg ggaagggact ggctgctatt gggcgaagtg 4740 ccggggcagg atctcctgtc atctcacctt gctcctgccg agaaagtatc catcatggct 4800 gatgcaatgc ggcggctgca tacgcttgat ccggctacct gcccattcga ccaccaagcg 4860 aaacatcgca tcgagcgagc acgtactcgg atggaagccg gtcttgtcga tcaggatgat 4920 ctggacgaag agcatcaggg gctcgcgcca gccgaactgt tcgccaggct caaggcgcgc 4980 atgcccgacg gcgaggatct cgtcgtgacc catggcgatg cctgcttgcc gaatatcatg 5040 gtggaaaatg gccgcttttc tggattcatc gactgtggcc ggctgggtgt ggcggaccgc 5100 tatcaggaca tagcgttggc tacccgtgat attgctgaag agcttggcgg cgaatgggct 5160 gaccgcttcc tcgtgcttta cggtatcgcc gctcccgatt cgcagcgcat cgccttctat 5220 cgccttcttg acgagttctt ctgaggggat cgatccgctg taagtctgca gaaattgatg 5280 atctattaaa caataaagat gtccactaaa atggaagttt ttcctgtcat actttgttaa 5340 gaagggtgag aacagagtac ctacattttg aatggaagga ttggagctac gggggtgggg 5400 gtggggtggg attagataaa tgcctgctct ttactgaagg ctctttacta ttgctttatg 5460 ataatgtttc atagttggat atcataattt aaacaagcaa aaccaaatta agggccagct 5520 cattcctccc actcatgatc tatagatcta tagatctctc gtgggatcat tgtttttctc 5580 ttgattccca ctttgtggtt ctaagtactg tggtttccaa atgtgtcagt ttcatagcct 5640 gaagaacgag atcagcagcc tctgttccac atacacttca ttctcagtat tgttttgcca 5700 agttctaatt ccatcagaag ctgactctag atcccgcgcc gaagttccta tactttctag 5760 agaataggaa cttcggaata ggaacttcaa gcttaagcgc tagaagatgg gcgggagtct 5820 tctgggcagg cttaaaggct aacctggtgt gtgggcgttg tcctgcaggg gaattgaaca 5880 ggtgtaaaat tggagggaca agacttccca cagattttcg gttttgtcgg gaagtttttt 5940 aataggggca aataaggaaa atgggaggat aggtagtcat ctggggtttt atgcagcaaa 6000 actacaggtt attattgctt gtgatccgcc tcggagtatt ttccatcgag gtagattaaa 6060 gacatgctca cccgagtttt atactctcct gcttgagatc cttactacag tatgaaatta 6120 cagtgtcgcg agttagacta tgtaagcaga attttaatca tttttaaaga gcccagtact 6180 tcatatccat ttctcccgct ccttctgcag ccttatcaaa aggtatttta gaacactcat 6240 tttagcccca ttttcattta ttatactggc ttatccaacc cctagacaga gcattggcat 6300 tttccctttc ctgatcttag aagtctgatg actcatgaaa ccagacagat tagttacata 6360 caccacaaat cgaggctgta gctggggcct caacactgca gttcttttat aactccttag 6420 tacacttttt gttgatcctt tgccttgatc cttaattttc agtgtctatc acctctcccg 6480 tcagtggtgt tccacatttg ggcctattct cagtccaggg agttttacaa caatagatgt 6540 attgagaatc caacctaaag cttaactttc cactcccatg aatgcctctc tcctttttct 6600 ccatttataa actgagctat taaccattaa tggttccagg tggatgtctc ctccccatat 6660 tacctgatgt atcttacata ttgccaggct gatattttaa gacattaaaa ggtatatttc 6720 attattgagc cacatggtat tgattactgc ttactaaaat tttgtcattg tacacatctg 6780 taaaaggtgg ttccttttgg aatgcaaagt tcaggtgttt gttgtctttc ctgacctaag 6840 gtcttgtgag cttgtatttt ttctatttaa gcagtgcttt ctcttggact ggcttgactc 6900 atggcattct acacgttatt gctggtctaa atgtgatttt gccaagcttc ttcaggacct 6960 ataattttgc ttgacttgta gccaaacaca agtaaaatga ttaagcaaca aatgtatttg 7020 tgaagcttgg tttttaggtt gttgtgttgt gtgtgcttgt gctctataat aatactatcc 7080 aggggctgga gaggtggctc ggagttcaag agcacagact gctcttccag aagtcctgag 7140 ttcaattccc agcaaccaca tggtggctca caaccatctg taatgggatc tgatgccctc 7200 ttctggtgtg tctgaagacc acaagtgtat tcacattaaa taaataaatc ctccttcttc 7260 ttcttttttt tttttttaaa gagaatactg tctccagtag aatttactga agtaatgaaa 7320 tactttgtgt ttgttccaat atggtagcca ataatcaaat tactctttaa gcactggaaa 7380 tgttaccaag gaactaattt ttatttgaag tgtaactgtg gacagaggag ccataactgc 7440 agacttgtgg gatacagaag accaatgcag actttaatgt cttttctctt acactaagca 7500 ataaagaaat aaaaattgaa cttctagtat cctatttgtt taaactgcta gctttactta 7560 acttttgtgc ttcatctata caaagctgaa agctaagtct gcagccatta ctaaacatga 7620 aagcaagtaa tgataatttt ggatttcaaa aatgtagggc cagagtttag ccagccagtg 7680 gtggtgcttg cctttatgcc tttaatccca gcactctgga ggcagagaca ggcagatctc 7740 tgagtttgag cccagcctgg tctacacatc aagttctatc taggatagcc aggaatacac 7800 acagaaaccc tgttggggag gggggctctg agatttcata aaattataat tgaagcattc 7860 cctaatgagc cactatggat gtggctaaat ccgtctacct ttctgatgag atttgggtat 7920 tattttttct gtctctgctg ttggttgggt cttttgacac tgtgggcttt ctttaaagcc 7980 tccttcctgc catgtggtct cttgtttgct actaacttcc catggcttaa atggcatggc 8040 tttttgcctt ctaagggcag ctgctgagat ttgcagcctg atttccaggg tggggttggg 8100 aaatctttca aacactaaaa ttgtccttta attttttttt taaaaaatgg gttatataat 8160 aaacctcata aaatagttat gaggagtgag gtggactaat attaaatgag tccctcccct 8220 ataaaagagc tattaaggct ttttgtctta tacttaactt tttttttaaa tgtggtatct 8280 ttagaaccaa gggtcttaga gttttagtat acagaaactg ttgcatcgct taatcagatt 8340 ttctagtttc aaatccagag aatccaaatt cttcacagcc aaagtcaaat taagaatttc 8400 tgacttttaa tgttaatttg cttactgtga atataaaaat gatagctttt cctgaggcag 8460 ggtctcacta tgtatctctg cctgatctgc aacaagatat gtagactaaa gttctgcctg 8520 cttttgtctc ctgaatacta aggttaaaat gtagtaatac ttttggaact tgcaggtcag 8580 attcttttat aggggacaca ctaagggagc ttgggtgata gttggtaaaa tgtgtttcaa 8640 gtgatgaaaa cttgaattat tatcaccgca acctactttt taaaaaaaaa agccaggcct 8700 gttagagcat gcttaaggga tccctaggac ttgctgagca cacaagagta gttacttggc 8760 aggctcctgg tgagagcata tttcaaaaaa caaggcagac aaccaagaaa ctacagttaa 8820 ggttacctgt ctttaaacca tctgcatata cacagggata ttaaaatatt ccaaataata 8880 tttcattcaa gttttccccc atcaaattgg gacatggatt tctccggtga ataggcagag 8940 ttggaaacta aacaaatgtt ggttttgtga tttgtgaaat tgttttcaag tgatagttaa 9000 agcccatgag atacagaaca aagctgctat ttcgaggtct cttggtttat actcagaagc 9060 acttctttgg gtttccctgc actatcctga tcatgtgcta ggcctacctt aggctgattg 9120 ttgttcaaat aaacttaagt ttcctgtcag gtgatgtcat atgatttcat atatcaaggc 9180 aaaacatgtt atatatgtta aacatttgta cttaatgtga aagttaggtc tttgtgggtt 9240 tgatttttaa ttttcaaaac ctgagctaaa taagtcattt ttacatgtct tacatttggt 9300 ggaattgtat aattgtggtt tgcaggcaag actctctgac ctagtaaccc tacctataga 9360 gcactttgct gggtcacaag tctaggagtc aagcatttca ccttgaagtt gagacgtttt 9420 gttagtgtat actagtttat atgttggagg acatgtttat ccagaagata ttcaggacta 9480 tttttgactg ggctaaggaa ttgattctga ttagcactgt tagtgagcat tgagtggcct 9540 ttaggcttga attggagtca cttgtatatc tcaaataatg ctggcctttt ttaaaaagcc 9600 cttgttcttt atcaccctgt tttctacata atttttgttc aaagaaatac ttgtttggat 9660 ctccttttga caacaatagc atgttttcaa gccatatttt ttttcctttt tttttttttt 9720 tttggttttt cgagacaggg tttctctgta tagccctggc tgtcctggaa ctcactttgt 9780 agaccaggct ggcctcgaac tcagaaatcc gcctgcctct gcctcctgag tgccgggatt 9840 aaaggcgtgc accaccacgc ctggctaagt tggatatttt gttatataac tataaccaat 9900 actaactcca ctgggtggat ttttaattca gtcagtagtc ttaagtggtc tttattggcc 9960 cttcattaaa atctactgtt cactctaaca gaggctgttg gtactagtgg cacttaagca 10020 acttcctacg gatatactag cagattaagg gtcagggata gaaactagtc tagcgttttg 10080 tatacctacc agctttatac taccttgttc tgatagaaat atttcaggac atctagcacc 10140 caattcgccc tatagtgagt cgtattacaa ttcactggcc gtcgttttac aacgtcgtga 10200 ctgggaaaac cctggcgtta cccaacttaa tcgccttgca gcacatcccc ctttcgccag 10260 ctggcgtaat agcgaagagg cccgcaccga tcgcccttcc caacagttgc gcagcctgaa 10320 tggcgaatgg gacgcgccct gtagcggcgc attaagcgcg gcgggtgtgg tggttacgcg 10380 cagcgtgacc gctacacttg ccagcgccct agcgcccgct cctttcgctt tcttcccttc 10440 ctttctcgcc acgttcgccg gctttccccg tcaagctcta aatcgggggc tccctttagg 10500 gttccgattt agtgctttac ggcacctcga ccccaaaaaa cttgattagg gtgatggttc 10560 acgtagtggg ccatcgccct gatagacggt ttttcgccct ttgacgttgg agtccacgtt 10620 ctttaatagt ggactcttgt tccaaactgg aacaacactc aaccctatct cggtctattc 10680 ttttgattta taagggattt tgccgatttc ggcctattgg ttaaaaaatg agctgattta 10740 acaaaaattt aacgcgaatt ttaacaaaat attaacgctt acaatttagg tggcactttt 10800 cggggaaatg tgcgcggaac ccctatttgt ttatttttct aaatacattc aaatatgtat 10860 ccgctcatga gacaataacc ctgataaatg cttcaataat attgaaaaag gaagagtatg 10920 agtattcaac atttccgtgt cgcccttatt cccttttttg cggcattttg ccttcctgtt 10980 tttgctcacc cagaaacgct ggtgaaagta aaagatgctg aagatcagtt gggtgcacga 11040 gtgggttaca tcgaactgga tctcaacagc ggtaagatcc ttgagagttt tcgccccgaa 11100 gaacgttttc caatgatgag cacttttaaa gttctgctat gtggcgcggt attatcccgt 11160 attgacgccg ggcaagagca actcggtcgc cgcatacact attctcagaa tgacttggtt 11220 gagtactcac cagtcacaga aaagcatctt acggatggca tgacagtaag agaattatgc 11280 agtgctgcca taaccatgag tgataacact gcggccaact tacttctgac aacgatcgga 11340 ggaccgaagg agctaaccgc ttttttgcac aacatggggg atcatgtaac tcgccttgat 11400 cgttgggaac cggagctgaa tgaagccata ccaaacgacg agcgtgacac cacgatgcct 11460 gtagcaatgg caacaacgtt gcgcaaacta ttaactggcg aactacttac tctagcttcc 11520 cggcaacaat taatagactg gatggaggcg gataaagttg caggaccact tctgcgctcg 11580 gcccttccgg ctggctggtt tattgctgat aaatctggag ccggtgagcg tgggtctcgc 11640 ggtatcattg cagcactggg gccagatggt aagccctccc gtatcgtagt tatctacacg 11700 acggggagtc aggcaactat ggatgaacga aatagacaga tcgctgagat aggtgcctca 11760 ctgattaagc attggtaact gtcagaccaa gtttactcat atatacttta gattgattta 11820 aaacttcatt tttaatttaa aaggatctag gtgaagatcc tttttgataa tctcatgacc 11880 aaaatccctt aacgtgagtt ttcgttccac tgagcgtcag accccgtaga aaagatcaaa 11940 ggatcttctt gagatccttt ttttctgcgc gtaatctgct gcttgcaaac aaaaaaacca 12000 ccgctaccag cggtggtttg tttgccggat caagagctac caactctttt tccgaaggta 12060 actggcttca gcagagcgca gataccaaat actgtccttc tagtgtagcc gtagttaggc 12120 caccacttca agaactctgt agcaccgcct acatacctcg ctctgctaat cctgttacca 12180 gtggctgctg ccagtggcga taagtcgtgt cttaccgggt tggactcaag acgatagtta 12240 ccggataagg cgcagcggtc gggctgaacg gggggttcgt gcacacagcc cagcttggag 12300 cgaacgacct acaccgaact gagataccta cagcgtgagc tatgagaaag cgccacgctt 12360 cccgaaggga gaaaggcgga caggtatccg gtaagcggca gggtcggaac aggagagcgc 12420 acgagggagc ttccaggggg aaacgcctgg tatctttata gtcctgtcgg gtttcgccac 12480 ctctgacttg agcgtcgatt tttgtgatgc tcgtcagggg ggcggagcct atggaaaaac 12540 gccagcaacg cggccttttt acggttcctg gccttttgct ggccttttgc tcacatgttc 12600 tttcctgcgt tatcccctga ttctgtggat aaccgtatta ccgcc 12645 14 23 DNA Artificial Oligonucleotide 14 gacaggacag tgcttgttta agg 23 15 23 DNA Artificial Oligonucleotide 15 tgactacaca atattgctcg cac 23 16 1073 DNA ROSA 5′ 16 caggccctcc gagcgtggtg gagccgttct gtgagacagc cgggtacgag tcgtgacgct 60 ggaaggggca agcgggtggt gggcaggaat gcggtccgcc ctgcagcaac cggaggggga 120 gggagaaggg agcggaaaag tctccaccgg acgcggccat ggctcggggg ggggggggca 180 gcggaggagc gcttccggcc gacgtctcgt cgctgattgg cttcttttcc tcccgccgtg 240 tgtgaaaaca caaatggcgt gttttggttg gcgtaaggcg cctgtcagtt aacggcagcc 300 ggagtgcgca gccgccggca gcctcgctct gcccactggg tggggcggga ggtaggtggg 360 gtgaggcgag ctggacgtgc gggcgcggtc ggcctctggc ggggcggggg aggggaggga 420 gggtcagcga aagtagctcg cgcgcgagcg gccgcccacc ctccccttcc tctgggggag 480 tcgttttacc cgccgccggc cgggcctcgt cgtctgattg gctctcgggg cccagaaaac 540 tggcccttgc cattggctcg tgttcgtgca agttgagtcc atccgccggc cagcgggggc 600 ggcgaggagg cgctcccagg ttccggccct cccctcggcc ccgcgccgca gagtctggcc 660 gcgcgcccct gcgcaacgtg gcaggaagcg cgcgctgggg gcggggacgg gcagtagggc 720 tgagcggctg cggggcgggt gcaagcacgt ttccgacttg agttgcctca agaggggcgt 780 gctgagccag acctccatcg cgcactccgg ggagtggagg gaaggagcga gggctcagtt 840 gggctgtttt ggaggcagga agcacttgct ctcccaaagt cgctctgagt tgttatcagt 900 aagggagctg cagtggagta ggcggggaga aggccgcacc cttctccgga ggggggaggg 960 gagtgttgca atacctttct gggagttctc tgctgcctcc tggcttctga ggaccgccct 1020 gggcctggga gaatcccttc cccctcttcc ctcgtgatct gcaactccag tct 1073 17 4333 DNA ROSA 3′ 17 tagaagatgg gcgggagtct tctgggcagg cttaaaggct aacctggtgt gtgggcgttg 60 tcctgcaggg gaattgaaca ggtgtaaaat tggagggaca agacttccca cagattttcg 120 gttttgtcgg gaagtttttt aataggggca aataaggaaa atgggaggat aggtagtcat 180 ctggggtttt atgcagcaaa actacaggtt attattgctt gtgatccgcc tcggagtatt 240 ttccatcgag gtagattaaa gacatgctca cccgagtttt atactctcct gcttgagatc 300 cttactacag tatgaaatta cagtgtcgcg agttagacta tgtaagcaga attttaatca 360 tttttaaaga gcccagtact tcatatccat ttctcccgct ccttctgcag ccttatcaaa 420 aggtatttta gaacactcat tttagcccca ttttcattta ttatactggc ttatccaacc 480 cctagacaga gcattggcat tttccctttc ctgatcttag aagtctgatg actcatgaaa 540 ccagacagat tagttacata caccacaaat cgaggctgta gctggggcct caacactgca 600 gttcttttat aactccttag tacacttttt gttgatcctt tgccttgatc cttaattttc 660 agtgtctatc acctctcccg tcagtggtgt tccacatttg ggcctattct cagtccaggg 720 agttttacaa caatagatgt attgagaatc caacctaaag cttaactttc cactcccatg 780 aatgcctctc tcctttttct ccatttataa actgagctat taaccattaa tggttccagg 840 tggatgtctc ctccccatat tacctgatgt atcttacata ttgccaggct gatattttaa 900 gacattaaaa ggtatatttc attattgagc cacatggtat tgattactgc ttactaaaat 960 tttgtcattg tacacatctg taaaaggtgg ttccttttgg aatgcaaagt tcaggtgttt 1020 gttgtctttc ctgacctaag gtcttgtgag cttgtatttt ttctatttaa gcagtgcttt 1080 ctcttggact ggcttgactc atggcattct acacgttatt gctggtctaa atgtgatttt 1140 gccaagcttc ttcaggacct ataattttgc ttgacttgta gccaaacaca agtaaaatga 1200 ttaagcaaca aatgtatttg tgaagcttgg tttttaggtt gttgtgttgt gtgtgcttgt 1260 gctctataat aatactatcc aggggctgga gaggtggctc ggagttcaag agcacagact 1320 gctcttccag aagtcctgag ttcaattccc agcaaccaca tggtggctca caaccatctg 1380 taatgggatc tgatgccctc ttctggtgtg tctgaagacc acaagtgtat tcacattaaa 1440 taaataaatc ctccttcttc ttcttttttt tttttttaaa gagaatactg tctccagtag 1500 aatttactga agtaatgaaa tactttgtgt ttgttccaat atggtagcca ataatcaaat 1560 tactctttaa gcactggaaa tgttaccaag gaactaattt ttatttgaag tgtaactgtg 1620 gacagaggag ccataactgc agacttgtgg gatacagaag accaatgcag actttaatgt 1680 cttttctctt acactaagca ataaagaaat aaaaattgaa cttctagtat cctatttgtt 1740 taaactgcta gctttactta acttttgtgc ttcatctata caaagctgaa agctaagtct 1800 gcagccatta ctaaacatga aagcaagtaa tgataatttt ggatttcaaa aatgtagggc 1860 cagagtttag ccagccagtg gtggtgcttg cctttatgcc tttaatccca gcactctgga 1920 ggcagagaca ggcagatctc tgagtttgag cccagcctgg tctacacatc aagttctatc 1980 taggatagcc aggaatacac acagaaaccc tgttggggag gggggctctg agatttcata 2040 aaattataat tgaagcattc cctaatgagc cactatggat gtggctaaat ccgtctacct 2100 ttctgatgag atttgggtat tattttttct gtctctgctg ttggttgggt cttttgacac 2160 tgtgggcttt ctttaaagcc tccttcctgc catgtggtct cttgtttgct actaacttcc 2220 catggcttaa atggcatggc tttttgcctt ctaagggcag ctgctgagat ttgcagcctg 2280 atttccaggg tggggttggg aaatctttca aacactaaaa ttgtccttta attttttttt 2340 taaaaaatgg gttatataat aaacctcata aaatagttat gaggagtgag gtggactaat 2400 attaaatgag tccctcccct ataaaagagc tattaaggct ttttgtctta tacttaactt 2460 tttttttaaa tgtggtatct ttagaaccaa gggtcttaga gttttagtat acagaaactg 2520 ttgcatcgct taatcagatt ttctagtttc aaatccagag aatccaaatt cttcacagcc 2580 aaagtcaaat taagaatttc tgacttttaa tgttaatttg cttactgtga atataaaaat 2640 gatagctttt cctgaggcag ggtctcacta tgtatctctg cctgatctgc aacaagatat 2700 gtagactaaa gttctgcctg cttttgtctc ctgaatacta aggttaaaat gtagtaatac 2760 ttttggaact tgcaggtcag attcttttat aggggacaca ctaagggagc ttgggtgata 2820 gttggtaaaa tgtgtttcaa gtgatgaaaa cttgaattat tatcaccgca acctactttt 2880 taaaaaaaaa agccaggcct gttagagcat gcttaaggga tccctaggac ttgctgagca 2940 cacaagagta gttacttggc aggctcctgg tgagagcata tttcaaaaaa caaggcagac 3000 aaccaagaaa ctacagttaa ggttacctgt ctttaaacca tctgcatata cacagggata 3060 ttaaaatatt ccaaataata tttcattcaa gttttccccc atcaaattgg gacatggatt 3120 tctccggtga ataggcagag ttggaaacta aacaaatgtt ggttttgtga tttgtgaaat 3180 tgttttcaag tgatagttaa agcccatgag atacagaaca aagctgctat ttcgaggtct 3240 cttggtttat actcagaagc acttctttgg gtttccctgc actatcctga tcatgtgcta 3300 ggcctacctt aggctgattg ttgttcaaat aaacttaagt ttcctgtcag gtgatgtcat 3360 atgatttcat atatcaaggc aaaacatgtt atatatgtta aacatttgta cttaatgtga 3420 aagttaggtc tttgtgggtt tgatttttaa ttttcaaaac ctgagctaaa taagtcattt 3480 ttacatgtct tacatttggt ggaattgtat aattgtggtt tgcaggcaag actctctgac 3540 ctagtaaccc tacctataga gcactttgct gggtcacaag tctaggagtc aagcatttca 3600 ccttgaagtt gagacgtttt gttagtgtat actagtttat atgttggagg acatgtttat 3660 ccagaagata ttcaggacta tttttgactg ggctaaggaa ttgattctga ttagcactgt 3720 tagtgagcat tgagtggcct ttaggcttga attggagtca cttgtatatc tcaaataatg 3780 ctggcctttt ttaaaaagcc cttgttcttt atcaccctgt tttctacata atttttgttc 3840 aaagaaatac ttgtttggat ctccttttga caacaatagc atgttttcaa gccatatttt 3900 ttttcctttt tttttttttt tttggttttt cgagacaggg tttctctgta tagccctggc 3960 tgtcctggaa ctcactttgt agaccaggct ggcctcgaac tcagaaatcc gcctgcctct 4020 gcctcctgag tgccgggatt aaaggcgtgc accaccacgc ctggctaagt tggatatttt 4080 gttatataac tataaccaat actaactcca ctgggtggat ttttaattca gtcagtagtc 4140 ttaagtggtc tttattggcc cttcattaaa atctactgtt cactctaaca gaggctgttg 4200 gtactagtgg cacttaagca acttcctacg gatatactag cagattaagg gtcagggata 4260 gaaactagtc tagcgttttg tatacctacc agctttatac taccttgttc tgatagaaat 4320 atttcaggac atc 4333 18 10491 DNA pROSA 12 18 tttgagtgag ctgataccgc tcgccgcagc cgaacgaccg agcgcagcga gtcagtgagc 60 gaggaagcgg aagagcgccc aatacgcaaa ccgcctctcc ccgcgcgttg gccgattcat 120 taatgcagct ggcacgacag gtttcccgac tggaaagcgg gcagtgagcg caacgcaatt 180 aatgtgagtt agctcactca ttaggcaccc caggctttac actttatgct tccggctcgt 240 atgttgtgtg gaattgtgag cggataacaa tttcacacag gaaacagcta tgaccatgat 300 tacgccaagc gcgcaattaa ccctcactaa agggaacaaa agctgtcgag atctagatat 360 cgatggccat agagttacgc tagggataac agggtaatat agccgcggca ggccctccga 420 gcgtggtgga gccgttctgt gagacagccg ggtacgagtc gtgacgctgg aaggggcaag 480 cgggtggtgg gcaggaatgc ggtccgccct gcagcaaccg gagggggagg gagaagggag 540 cggaaaagtc tccaccggac gcggccatgg ctcggggggg ggggggcagc ggaggagcgc 600 ttccggccga cgtctcgtcg ctgattggct tcttttcctc ccgccgtgtg tgaaaacaca 660 aatggcgtgt tttggttggc gtaaggcgcc tgtcagttaa cggcagccgg agtgcgcagc 720 cgccggcagc ctcgctctgc ccactgggtg gggcgggagg taggtggggt gaggcgagct 780 ggacgtgcgg gcgcggtcgg cctctggcgg ggcgggggag gggagggagg gtcagcgaaa 840 gtagctcgcg cgcgagcggc cgcccaccct ccccttcctc tgggggagtc gttttacccg 900 ccgccggccg ggcctcgtcg tctgattggc tctcggggcc cagaaaactg gcccttgcca 960 ttggctcgtg ttcgtgcaag ttgagtccat ccgccggcca gcgggggcgg cgaggaggcg 1020 ctcccaggtt ccggccctcc cctcggcccc gcgccgcaga gtctggccgc gcgcccctgc 1080 gcaacgtggc aggaagcgcg cgctgggggc ggggacgggc agtagggctg agcggctgcg 1140 gggcgggtgc aagcacgttt ccgacttgag ttgcctcaag aggggcgtgc tgagccagac 1200 ctccatcgcg cactccgggg agtggaggga aggagcgagg gctcagttgg gctgttttgg 1260 aggcaggaag cacttgctct cccaaagtcg ctctgagttg ttatcagtaa gggagctgca 1320 gtggagtagg cggggagaag gccgcaccct tctccggagg ggggagggga gtgttgcaat 1380 acctttctgg gagttctctg ctgcctcctg gcttctgagg accgccctgg gcctgggaga 1440 atcccttccc cctcttccct cgtgatctgc aactccagtc tttctaggta accgatatcc 1500 ctgcaggggt gacctgcacg tctagggcgc agtagtccag ggtttccttg atgatgtcat 1560 acttatcctg tccctttttt ttccacagct cgcggttgag gacaaactct tcgcggtctt 1620 tccagtactc ctgcaggtga ctgactgagt cgacttaatt aaggccatag cggccattta 1680 aatcggccgg cctaggcgcg ccggtaaccg aagttcctat actttctaga gaataggaac 1740 ttcggaatag gaacttctta ggtcaattct accgggtagg ggaggcgctt ttcccaaggc 1800 agtctggagc atgcgcttta gcagccccgc tgggcacttg gcgctacaca agtggcctct 1860 ggcctcgcac acattccaca tccaccggta ggcgccaacc ggctccgttc tttggtggcc 1920 ccttcgcgcc accttctact cctcccctag tcaggaagtt cccccccgcc ccgcagctcg 1980 cgtcgtgcag gacgtgacaa atggaagtag cacgtctcac tagtctcgtg cagatggaca 2040 gcaccgctga gcaatggaag cgggtaggcc tttggggcag cggccaatag cagctttgct 2100 ccttcgcttt ctgggctcag aggctgggaa ggggtgggtc cgggggcggg ctcaggggcg 2160 ggctcagggg cggggcgggc gcccgaaggt cctccggagg cccggcattc tgcacgcttc 2220 aaaagcgcac gtctgccgcg ctgttctcct cttcctcatc tccgggcctt tcgacctgca 2280 gccaatatgg gatcggccat tgaacaagat ggattgcacg caggttctcc ggccgcttgg 2340 gtggagaggc tattcggcta tgactgggca caacagacaa tcggctgctc tgatgccgcc 2400 gtgttccggc tgtcagcgca ggggcgcccg gttctttttg tcaagaccga cctgtccggt 2460 gccctgaatg aactgcagga cgaggcagcg cggctatcgt ggctggccac gacgggcgtt 2520 ccttgcgcag ctgtgctcga cgttgtcact gaagcgggaa gggactggct gctattgggc 2580 gaagtgccgg ggcaggatct cctgtcatct caccttgctc ctgccgagaa agtatccatc 2640 atggctgatg caatgcggcg gctgcatacg cttgatccgg ctacctgccc attcgaccac 2700 caagcgaaac atcgcatcga gcgagcacgt actcggatgg aagccggtct tgtcgatcag 2760 gatgatctgg acgaagagca tcaggggctc gcgccagccg aactgttcgc caggctcaag 2820 gcgcgcatgc ccgacggcga ggatctcgtc gtgacccatg gcgatgcctg cttgccgaat 2880 atcatggtgg aaaatggccg cttttctgga ttcatcgact gtggccggct gggtgtggcg 2940 gaccgctatc aggacatagc gttggctacc cgtgatattg ctgaagagct tggcggcgaa 3000 tgggctgacc gcttcctcgt gctttacggt atcgccgctc ccgattcgca gcgcatcgcc 3060 ttctatcgcc ttcttgacga gttcttctga ggggatcgat ccgctgtaag tctgcagaaa 3120 ttgatgatct attaaacaat aaagatgtcc actaaaatgg aagtttttcc tgtcatactt 3180 tgttaagaag ggtgagaaca gagtacctac attttgaatg gaaggattgg agctacgggg 3240 gtgggggtgg ggtgggatta gataaatgcc tgctctttac tgaaggctct ttactattgc 3300 tttatgataa tgtttcatag ttggatatca taatttaaac aagcaaaacc aaattaaggg 3360 ccagctcatt cctcccactc atgatctata gatctataga tctctcgtgg gatcattgtt 3420 tttctcttga ttcccacttt gtggttctaa gtactgtggt ttccaaatgt gtcagtttca 3480 tagcctgaag aacgagatca gcagcctctg ttccacatac acttcattct cagtattgtt 3540 ttgccaagtt ctaattccat cagaagctga ctctagatcc cgcgccgaag ttcctatact 3600 ttctagagaa taggaacttc ggaataggaa cttcaagctt aagcgctaga agatgggcgg 3660 gagtcttctg ggcaggctta aaggctaacc tggtgtgtgg gcgttgtcct gcaggggaat 3720 tgaacaggtg taaaattgga gggacaagac ttcccacaga ttttcggttt tgtcgggaag 3780 ttttttaata ggggcaaata aggaaaatgg gaggataggt agtcatctgg ggttttatgc 3840 agcaaaacta caggttatta ttgcttgtga tccgcctcgg agtattttcc atcgaggtag 3900 attaaagaca tgctcacccg agttttatac tctcctgctt gagatcctta ctacagtatg 3960 aaattacagt gtcgcgagtt agactatgta agcagaattt taatcatttt taaagagccc 4020 agtacttcat atccatttct cccgctcctt ctgcagcctt atcaaaaggt attttagaac 4080 actcatttta gccccatttt catttattat actggcttat ccaaccccta gacagagcat 4140 tggcattttc cctttcctga tcttagaagt ctgatgactc atgaaaccag acagattagt 4200 tacatacacc acaaatcgag gctgtagctg gggcctcaac actgcagttc ttttataact 4260 ccttagtaca ctttttgttg atcctttgcc ttgatcctta attttcagtg tctatcacct 4320 ctcccgtcag tggtgttcca catttgggcc tattctcagt ccagggagtt ttacaacaat 4380 agatgtattg agaatccaac ctaaagctta actttccact cccatgaatg cctctctcct 4440 ttttctccat ttataaactg agctattaac cattaatggt tccaggtgga tgtctcctcc 4500 ccatattacc tgatgtatct tacatattgc caggctgata ttttaagaca ttaaaaggta 4560 tatttcatta ttgagccaca tggtattgat tactgcttac taaaattttg tcattgtaca 4620 catctgtaaa aggtggttcc ttttggaatg caaagttcag gtgtttgttg tctttcctga 4680 cctaaggtct tgtgagcttg tattttttct atttaagcag tgctttctct tggactggct 4740 tgactcatgg cattctacac gttattgctg gtctaaatgt gattttgcca agcttcttca 4800 ggacctataa ttttgcttga cttgtagcca aacacaagta aaatgattaa gcaacaaatg 4860 tatttgtgaa gcttggtttt taggttgttg tgttgtgtgt gcttgtgctc tataataata 4920 ctatccaggg gctggagagg tggctcggag ttcaagagca cagactgctc ttccagaagt 4980 cctgagttca attcccagca accacatggt ggctcacaac catctgtaat gggatctgat 5040 gccctcttct ggtgtgtctg aagaccacaa gtgtattcac attaaataaa taaatcctcc 5100 ttcttcttct tttttttttt tttaaagaga atactgtctc cagtagaatt tactgaagta 5160 atgaaatact ttgtgtttgt tccaatatgg tagccaataa tcaaattact ctttaagcac 5220 tggaaatgtt accaaggaac taatttttat ttgaagtgta actgtggaca gaggagccat 5280 aactgcagac ttgtgggata cagaagacca atgcagactt taatgtcttt tctcttacac 5340 taagcaataa agaaataaaa attgaacttc tagtatccta tttgtttaaa ctgctagctt 5400 tacttaactt ttgtgcttca tctatacaaa gctgaaagct aagtctgcag ccattactaa 5460 acatgaaagc aagtaatgat aattttggat ttcaaaaatg tagggccaga gtttagccag 5520 ccagtggtgg tgcttgcctt tatgccttta atcccagcac tctggaggca gagacaggca 5580 gatctctgag tttgagccca gcctggtcta cacatcaagt tctatctagg atagccagga 5640 atacacacag aaaccctgtt ggggaggggg gctctgagat ttcataaaat tataattgaa 5700 gcattcccta atgagccact atggatgtgg ctaaatccgt ctacctttct gatgagattt 5760 gggtattatt ttttctgtct ctgctgttgg ttgggtcttt tgacactgtg ggctttcttt 5820 aaagcctcct tcctgccatg tggtctcttg tttgctacta acttcccatg gcttaaatgg 5880 catggctttt tgccttctaa gggcagctgc tgagatttgc agcctgattt ccagggtggg 5940 gttgggaaat ctttcaaaca ctaaaattgt cctttaattt tttttttaaa aaatgggtta 6000 tataataaac ctcataaaat agttatgagg agtgaggtgg actaatatta aatgagtccc 6060 tcccctataa aagagctatt aaggcttttt gtcttatact taactttttt tttaaatgtg 6120 gtatctttag aaccaagggt cttagagttt tagtatacag aaactgttgc atcgcttaat 6180 cagattttct agtttcaaat ccagagaatc caaattcttc acagccaaag tcaaattaag 6240 aatttctgac ttttaatgtt aatttgctta ctgtgaatat aaaaatgata gcttttcctg 6300 aggcagggtc tcactatgta tctctgcctg atctgcaaca agatatgtag actaaagttc 6360 tgcctgcttt tgtctcctga atactaaggt taaaatgtag taatactttt ggaacttgca 6420 ggtcagattc ttttataggg gacacactaa gggagcttgg gtgatagttg gtaaaatgtg 6480 tttcaagtga tgaaaacttg aattattatc accgcaacct actttttaaa aaaaaaagcc 6540 aggcctgtta gagcatgctt aagggatccc taggacttgc tgagcacaca agagtagtta 6600 cttggcaggc tcctggtgag agcatatttc aaaaaacaag gcagacaacc aagaaactac 6660 agttaaggtt acctgtcttt aaaccatctg catatacaca gggatattaa aatattccaa 6720 ataatatttc attcaagttt tcccccatca aattgggaca tggatttctc cggtgaatag 6780 gcagagttgg aaactaaaca aatgttggtt ttgtgatttg tgaaattgtt ttcaagtgat 6840 agttaaagcc catgagatac agaacaaagc tgctatttcg aggtctcttg gtttatactc 6900 agaagcactt ctttgggttt ccctgcacta tcctgatcat gtgctaggcc taccttaggc 6960 tgattgttgt tcaaataaac ttaagtttcc tgtcaggtga tgtcatatga tttcatatat 7020 caaggcaaaa catgttatat atgttaaaca tttgtactta atgtgaaagt taggtctttg 7080 tgggtttgat ttttaatttt caaaacctga gctaaataag tcatttttac atgtcttaca 7140 tttggtggaa ttgtataatt gtggtttgca ggcaagactc tctgacctag taaccctacc 7200 tatagagcac tttgctgggt cacaagtcta ggagtcaagc atttcacctt gaagttgaga 7260 cgttttgtta gtgtatacta gtttatatgt tggaggacat gtttatccag aagatattca 7320 ggactatttt tgactgggct aaggaattga ttctgattag cactgttagt gagcattgag 7380 tggcctttag gcttgaattg gagtcacttg tatatctcaa ataatgctgg ccttttttaa 7440 aaagcccttg ttctttatca ccctgttttc tacataattt ttgttcaaag aaatacttgt 7500 ttggatctcc ttttgacaac aatagcatgt tttcaagcca tatttttttt cctttttttt 7560 tttttttttg gtttttcgag acagggtttc tctgtatagc cctggctgtc ctggaactca 7620 ctttgtagac caggctggcc tcgaactcag aaatccgcct gcctctgcct cctgagtgcc 7680 gggattaaag gcgtgcacca ccacgcctgg ctaagttgga tattttgtta tataactata 7740 accaatacta actccactgg gtggattttt aattcagtca gtagtcttaa gtggtcttta 7800 ttggcccttc attaaaatct actgttcact ctaacagagg ctgttggtac tagtggcact 7860 taagcaactt cctacggata tactagcaga ttaagggtca gggatagaaa ctagtctagc 7920 gttttgtata cctaccagct ttatactacc ttgttctgat agaaatattt caggacatct 7980 agcacccaat tcgccctata gtgagtcgta ttacaattca ctggccgtcg ttttacaacg 8040 tcgtgactgg gaaaaccctg gcgttaccca acttaatcgc cttgcagcac atcccccttt 8100 cgccagctgg cgtaatagcg aagaggcccg caccgatcgc ccttcccaac agttgcgcag 8160 cctgaatggc gaatgggacg cgccctgtag cggcgcatta agcgcggcgg gtgtggtggt 8220 tacgcgcagc gtgaccgcta cacttgccag cgccctagcg cccgctcctt tcgctttctt 8280 cccttccttt ctcgccacgt tcgccggctt tccccgtcaa gctctaaatc gggggctccc 8340 tttagggttc cgatttagtg ctttacggca cctcgacccc aaaaaacttg attagggtga 8400 tggttcacgt agtgggccat cgccctgata gacggttttt cgccctttga cgttggagtc 8460 cacgttcttt aatagtggac tcttgttcca aactggaaca acactcaacc ctatctcggt 8520 ctattctttt gatttataag ggattttgcc gatttcggcc tattggttaa aaaatgagct 8580 gatttaacaa aaatttaacg cgaattttaa caaaatatta acgcttacaa tttaggtggc 8640 acttttcggg gaaatgtgcg cggaacccct atttgtttat ttttctaaat acattcaaat 8700 atgtatccgc tcatgagaca ataaccctga taaatgcttc aataatattg aaaaaggaag 8760 agtatgagta ttcaacattt ccgtgtcgcc cttattccct tttttgcggc attttgcctt 8820 cctgtttttg ctcacccaga aacgctggtg aaagtaaaag atgctgaaga tcagttgggt 8880 gcacgagtgg gttacatcga actggatctc aacagcggta agatccttga gagttttcgc 8940 cccgaagaac gttttccaat gatgagcact tttaaagttc tgctatgtgg cgcggtatta 9000 tcccgtattg acgccgggca agagcaactc ggtcgccgca tacactattc tcagaatgac 9060 ttggttgagt actcaccagt cacagaaaag catcttacgg atggcatgac agtaagagaa 9120 ttatgcagtg ctgccataac catgagtgat aacactgcgg ccaacttact tctgacaacg 9180 atcggaggac cgaaggagct aaccgctttt ttgcacaaca tgggggatca tgtaactcgc 9240 cttgatcgtt gggaaccgga gctgaatgaa gccataccaa acgacgagcg tgacaccacg 9300 atgcctgtag caatggcaac aacgttgcgc aaactattaa ctggcgaact acttactcta 9360 gcttcccggc aacaattaat agactggatg gaggcggata aagttgcagg accacttctg 9420 cgctcggccc ttccggctgg ctggtttatt gctgataaat ctggagccgg tgagcgtggg 9480 tctcgcggta tcattgcagc actggggcca gatggtaagc cctcccgtat cgtagttatc 9540 tacacgacgg ggagtcaggc aactatggat gaacgaaata gacagatcgc tgagataggt 9600 gcctcactga ttaagcattg gtaactgtca gaccaagttt actcatatat actttagatt 9660 gatttaaaac ttcattttta atttaaaagg atctaggtga agatcctttt tgataatctc 9720 atgaccaaaa tcccttaacg tgagttttcg ttccactgag cgtcagaccc cgtagaaaag 9780 atcaaaggat cttcttgaga tccttttttt ctgcgcgtaa tctgctgctt gcaaacaaaa 9840 aaaccaccgc taccagcggt ggtttgtttg ccggatcaag agctaccaac tctttttccg 9900 aaggtaactg gcttcagcag agcgcagata ccaaatactg tccttctagt gtagccgtag 9960 ttaggccacc acttcaagaa ctctgtagca ccgcctacat acctcgctct gctaatcctg 10020 ttaccagtgg ctgctgccag tggcgataag tcgtgtctta ccgggttgga ctcaagacga 10080 tagttaccgg ataaggcgca gcggtcgggc tgaacggggg gttcgtgcac acagcccagc 10140 ttggagcgaa cgacctacac cgaactgaga tacctacagc gtgagctatg agaaagcgcc 10200 acgcttcccg aagggagaaa ggcggacagg tatccggtaa gcggcagggt cggaacagga 10260 gagcgcacga gggagcttcc agggggaaac gcctggtatc tttatagtcc tgtcgggttt 10320 cgccacctct gacttgagcg tcgatttttg tgatgctcgt caggggggcg gagcctatgg 10380 aaaaacgcca gcaacgcggc ctttttacgg ttcctggcct tttgctggcc ttttgctcac 10440 atgttctttc ctgcgttatc ccctgattct gtggataacc gtattaccgc c 10491 19 448 DNA ROSA5.1 19 aaggatactg gggcatacgc cacagggagt ccaagaatgt gaggtggggg tggcgaaggt 60 aatgtctttg gtgtgggaaa agcagcagcc atctgagata ggaactggaa aaccagagga 120 gaggcgttca ggaagattat ggaggggagg actgggcccc cacgagcgac cagagttgtc 180 acaaggccgc aagaacaggg gaggtggggg gctcagggac agaaaaaaaa gtatgtgtat 240 tttgagagca gggttgggag gcctctcctg aaaagggtat aaacgtggag taggcaatac 300 ccaggcaaaa aggggagacc agagtagggg gaggggaaga gtcctgaccc agggaagaca 360 ttaaaaaggt agtggggtcg actagatgaa ggagagcctt tctctctggg caagagcggt 420 gcaatggtgt gtaaaggtag ctgagaag 448 20 11784 DNA C31 substrate reporter 20 ggcaggccct ccgagcgtgg tggagccgtt ctgtgagaca gccgggtacg agtcgtgacg 60 ctggaagggg caagcgggtg gtgggcagga atgcggtccg ccctgcagca accggagggg 120 gagggagaag ggagcggaaa agtctccacc ggacgcggcc atggctcggg gggggggggg 180 cagcggagga gcgcttccgg ccgacgtctc gtcgctgatt ggcttctttt cctcccgccg 240 tgtgtgaaaa cacaaatggc gtgttttggt tggcgtaagg cgcctgtcag ttaacggcag 300 ccggagtgcg cagccgccgg cagcctcgct ctgcccactg ggtggggcgg gaggtaggtg 360 gggtgaggcg agctggacgt gcgggcgcgg tcggcctctg gcggggcggg ggaggggagg 420 gagggtcagc gaaagtagct cgcgcgcgag cggccgccca ccctcccctt cctctggggg 480 agtcgtttta cccgccgccg gccgggcctc gtcgtctgat tggctctcgg ggcccagaaa 540 actggccctt gccattggct cgtgttcgtg caagttgagt ccatccgccg gccagcgggg 600 gcggcgagga ggcgctccca ggttccggcc ctcccctcgg ccccgcgccg cagagtctgg 660 ccgcgcgccc ctgcgcaacg tggcaggaag cgcgcgctgg gggcggggac gggcagtagg 720 gctgagcggc tgcggggcgg gtgcaagcac gtttccgact tgagttgcct caagaggggc 780 gtgctgagcc agacctccat cgcgcactcc ggggagtgga gggaaggagc gagggctcag 840 ttgggctgtt ttggaggcag gaagcacttg ctctcccaaa gtcgctctga gttgttatca 900 gtaagggagc tgcagtggag taggcgggga gaaggccgca cccttctccg gaggggggag 960 gggagtgttg caataccttt ctgggagttc tctgctgcct cctggcttct gaggaccgcc 1020 ctgggcctgg gagaatccct tccccctctt ccctcgtgat ctgcaactcc agtctttcgc 1080 ctaggtaacc gatatccctg caggggtgac ctgcacgtct agggcgcagt agtccagggt 1140 ttccttgatg atgtcatact tatcctgtcc cttttttttc cacagctcgc ggttgaggac 1200 aaactcttcg cggtctttcc agtactcctg caggtgactg actgagtcga cgacactgca 1260 gagacctact tcactaacaa ccggtacagt tcgtggacca gatgggtgag gtggagtacg 1320 cgcccgggga gcccaagggc acgccctggc acccgcaccg cggcttcgag accgtcacga 1380 ataacttcgt atagcataca ttatacgaag ttataagctc gatgaattct accgggtagg 1440 ggaggcgctt ttcccaaggc agtctggagc atgcgcttta gcagccccgc tggcacttgg 1500 cgctacacaa gtggcctctg gcctcgcaca cattccacat ccaccggtag cgccaaccgg 1560 ctccgttctt tggtggcccc ttcgcgccac cttctactcc tcccctagtc aggaagttcc 1620 cccccgcccc gcagctcgcg tcgtgcagga cgtgacaaat ggaagtagca cgtctcacta 1680 gtctcgtgca gatggacagc accgctgagc aatggaagcg ggtaggcctt tggggcagcg 1740 gccaatagca gctttgctcc ttcgctttct gggctcagag gctgggaagg ggtgggtccg 1800 ggggcgggct caggggcggg ctcaggggcg gggcgggcgc gaaggtcctc ccgaggcccg 1860 gcattctcgc acgcttcaaa agcgcacgtc tgccgcgctg ttctcctctt cctcatctcc 1920 gggcctttcg acgatccagc cgccaccatg aaaaagcctg aactcaccgc gacgtctgtc 1980 gagaagtttc tgatcgaaaa gttcgacagc gtctccgacc tgatgcagct ctcggagggc 2040 gaagaatctc gtgctttcag cttcgatgta ggagggcgtg gatatgtcct gcgggtaaat 2100 agctgcgccg atggtttcta caaagatcgt tatgtttatc ggcactttgc atcggccgcg 2160 ctcccgattc cggaagtgct tgacattggg gaattcagcg agagcctgac ctattgcatc 2220 tcccgccgtg cacagggtgt cacgttgcaa gacctgcctg aaaccgaact gcccgctgtt 2280 ctgcagccgg tcgcggaggc catggatgcg atcgctgcgg ccgatcttag ccagacgagc 2340 gggttcggcc cattcggacc gcaaggaatc ggtcaataca ctacatggcg tgatttcata 2400 tgcgcgattg ctgatcccca tgtgtatcac tggcaaactg tgatggacga caccgtcagt 2460 gcgtccgtcg cgcaggctct cgatgagctg atgctttggg ccgaggactg ccccgaagtc 2520 cggcacctcg tgcacgcgga tttcggctcc aacaatgtcc tgacggacaa tggccgcata 2580 acagcggtca ttgactggag cgaggcgatg ttcggggatt cccaatacga ggtcgccaac 2640 atcttcttct ggaggccgtg gttggcttgt atggagcagc agacgcgcta cttcgagcgg 2700 aggcatccgg agcttgcagg atcgccgcgg ctccgggcgt atatgctccg cattggtctt 2760 gaccaactct atcagagctt ggttgacggc aatttcgatg atgcagcttg ggcgcagggt 2820 cgatgcgacg caatcgtccg atccggagcc gggactgtcg ggcgtacaca aatcgcccgc 2880 agaagcgcgg ccgtctggac cgatggctgt gtagaagtac tcgccgatag tggaaaccga 2940 cgccccagca ctcgtccgag ggcaaaggaa tagtcgatgc agaaattgat gatctattaa 3000 acaataaaga tgtccactaa aatggaagtt tttcctgtca tactttgtta agaagggtga 3060 gaacagagta cctacatttt gaatggaagg attggagcta cgggggtggg ggtggggtgg 3120 gattagataa atgcctgctc tttactgaag gctctttact attgctttat gataatgttt 3180 catagttgga tatcataatt taaacaagca aaaccaaatt aagggccagc tcattcctcc 3240 cactcatgat ctatagatct atagatctct cgtgggatca ttgtttttct cttgattccc 3300 actttgtggt tctaagtact gtggtttcca aatgtgtcag tttcatagcc tgaagaacga 3360 gatcagcagc ctctgttcca catacacttc attctcagta ttgttttgcc aagttctaat 3420 tccatcagaa gcttcagctg ctcgactaga ggatcataat cagccatacc acatttgtag 3480 aggttttact tgctttaaaa aacctcccac acctccccct gaacctgaaa cataaaatga 3540 atgcaattgt tgttgttaac ttgtttattg cagcttataa tggttacaaa taaagcaata 3600 gcatcacaaa tttcacaaat aaagcatttt tttcactgca ttctagttgt ggtttgtcca 3660 aactcatcaa tgtatcttat catgtctgga tccgtgtcat gtcggcgacc ctacgccccc 3720 aactgagaga actcaaaggt taccccagtt ggggcactac tcccgaaaac cgcttctgga 3780 tccataactt cgtatagcat acattatacg aagttatacc gggccaccat ggtcgcgagt 3840 agcttggcac tggccgtcgt tttacaacgt cgtgactggg aaaaccctgg cgttacccaa 3900 cttaatcgcc ttgcagcaca tccccctttc gccagctggc gtaatagcga agaggcccgc 3960 accgatcgcc cttcccaaca gttgcgcagc ctgaatggcg aatggcgctt tgcctggttt 4020 ccggcaccag aagcggtgcc ggaaagctgg ctggagtgcg atcttcctga ggccgatact 4080 gtcgtcgtcc cctcaaactg gcagatgcac ggttacgatg cgcccatcta caccaacgta 4140 acctatccca ttacggtcaa tccgccgttt gttcccacgg agaatccgac gggttgttac 4200 tcgctcacat ttaatgttga tgaaagctgg ctacaggaag gccagacgcg aattattttt 4260 gatggcgtta actcggcgtt tcatctgtgg tgcaacgggc gctgggtcgg ttacggccag 4320 gacagtcgtt tgccgtctga atttgacctg agcgcatttt tacgcgccgg agaaaaccgc 4380 ctcgcggtga tggtgctgcg ttggagtgac ggcagttatc tggaagatca ggatatgtgg 4440 cggatgagcg gcattttccg tgacgtctcg ttgctgcata aaccgactac acaaatcagc 4500 gatttccatg ttgccactcg ctttaatgat gatttcagcc gcgctgtact ggaggctgaa 4560 gttcagatgt gcggcgagtt gcgtgactac ctacgggtaa cagtttcttt atggcagggt 4620 gaaacgcagg tcgccagcgg caccgcgcct ttcggcggtg aaattatcga tgagcgtggt 4680 ggttatgccg atcgcgtcac actacgtctg aacgtcgaaa acccgaaact gtggagcgcc 4740 gaaatcccga atctctatcg tgcggtggtt gaactgcaca ccgccgacgg cacgctgatt 4800 gaagcagaag cctgcgatgt cggtttccgc gaggtgcgga ttgaaaatgg tctgctgctg 4860 ctgaacggca agccgttgct gattcgaggc gttaaccgtc acgagcatca tcctctgcat 4920 ggtcaggtca tggatgagca gacgatggtg caggatatcc tgctgatgaa gcagaacaac 4980 tttaacgccg tgcgctgttc gcattatccg aaccatccgc tgtggtacac gctgtgcgac 5040 cgctacggcc tgtatgtggt ggatgaagcc aatattgaaa cccacggcat ggtgccaatg 5100 aatcgtctga ccgatgatcc gcgctggcta ccggcgatga gcgaacgcgt aacgcgaatg 5160 gtgcagcgcg atcgtaatca cccgagtgtg atcatctggt cgctggggaa tgaatcaggc 5220 cacggcgcta atcacgacgc gctgtatcgc tggatcaaat ctgtcgatcc ttcccgcccg 5280 gtgcagtatg aaggcggcgg agccgacacc acggccaccg atattatttg cccgatgtac 5340 gcgcgcgtgg atgaagacca gcccttcccg gctgtgccga aatggtccat caaaaaatgg 5400 ctttcgctac ctggagagac gcgcccgctg atcctttgcg aatacgccca cgcgatgggt 5460 aacagtcttg gcggtttcgc taaatactgg caggcgtttc gtcagtatcc ccgtttacag 5520 ggcggcttcg tctgggactg ggtggatcag tcgctgatta aatatgatga aaacggcaac 5580 ccgtggtcgg cttacggcgg tgattttggc gatacgccga acgatcgcca gttctgtatg 5640 aacggtctgg tctttgccga ccgcacgccg catccagcgc tgacggaagc aaaacaccag 5700 cagcagtttt tccagttccg tttatccggg caaaccatcg aagtgaccag cgaatacctg 5760 ttccgtcata gcgataacga gctcctgcac tggatggtgg cgctggatgg taagccgctg 5820 gcaagcggtg aagtgcctct ggatgtcgct ccacaaggta aacagttgat tgaactgcct 5880 gaactaccgc agccggagag cgccgggcaa ctctggctca cagtacgcgt agtgcaaccg 5940 aacgcgaccg catggtcaga agccgggcac atcagcgcct ggcagcagtg gcgtctggcg 6000 gaaaacctca gtgtgacgct ccccgccgcg tcccacgcca tcccgcatct gaccaccagc 6060 gaaatggatt tttgcatcga gctgggtaat aagcgttggc aatttaaccg ccagtcaggc 6120 tttctttcac agatgtggat tggcgataaa aaacaactgc tgacgccgct gcgcgatcag 6180 ttcacccgtg caccgctgga taacgacatt ggcgtaagtg aagcgacccg cattgaccct 6240 aacgcctggg tcgaacgctg gaaggcggcg ggccattacc aggccgaagc agcgttgttg 6300 cagtgcacgg cagatacact tgctgatgcg gtgctgatta cgaccgctca cgcgtggcag 6360 catcagggga aaaccttatt tatcagccgg aaaacctacc ggattgatgg tagtggtcaa 6420 atggcgatta ccgttgatgt tgaagtggcg agcgatacac cgcatccggc gcggattggc 6480 ctgaactgcc agctggcgca ggtagcagag cgggtaaact ggctcggatt agggccgcaa 6540 gaaaactatc ccgaccgcct tactgccgcc tgttttgacc gctgggatct gccattgtca 6600 gacatgtata ccccgtacgt cttcccgagc gaaaacggtc tgcgctgcgg gacgcgcgaa 6660 ttgaattatg gcccacacca gtggcgcggc gacttccagt tcaacatcag ccgctacagt 6720 caacagcaac tgatggaaac cagccatcgc catctgctgc acgcggaaga aggcacatgg 6780 ctgaatatcg acggtttcca tatggggatt ggtggcgacg actcctggag cccgtcagta 6840 tcggcggaat tccagctgag cgccggtcgc taccattacc agttggtctg gtgtcaaaaa 6900 taataataac cgggcagggg ggatctttgt gaaggaacct tacttctgtg gtgtgacata 6960 attggacaaa ctacctacag agatttaaag ctctaaggta aatataaaat ttttaagtgt 7020 ataatgtgtt aaactactga ttctaattgt ttgtgtattt tagattccaa cctatggaac 7080 tgatgaatgg gagcagtggt ggaatgccag atccagacat gataagatac attgatgagt 7140 ttggacaaac cacaactaga atgcagtgaa aaaaatgctt tatttgtgaa atttgtgatg 7200 ctattgcttt atttgtaacc attataagct gcaataaaca agttaacaac aacaattgca 7260 ttcattttat gtttcaggtt cagggggagg tgtgggaggt tttttaaagc aagtaaaacc 7320 tctacaaatg tggtatggct gattatgatc tgcggccaaa tcggccggcc taggcgcgcc 7380 ggtaaccgaa gttcctatac tttctagaga ataggaactt cggaatagga acttcaagct 7440 taagcgctag cctagaagat gggcgggagt cttctgggca ggcttaaagg ctaacctggt 7500 gtgtgggcgt tgtcctgcag gggaattgaa caggtgtaaa attggaggga caagacttcc 7560 cacagatttt cggttttgtc gggaagtttt ttaatagggg caaataagga aaatgggagg 7620 ataggtagtc atctggggtt ttatgcagca aaactacagg ttattattgc ttgtgatccg 7680 cctcggagta ttttccatcg aggtagatta aagacatgct cacccgagtt ttatactctc 7740 ctgcttgaga tccttactac agtatgaaat tacagtgtcg cgagttagac tatgtaagca 7800 gaattttaat catttttaaa gagcccagta cttcatatcc atttctcccg ctccttctgc 7860 agccttatca aaaggtattt tagaacactc attttagccc cattttcatt tattatactg 7920 gcttatccaa cccctagaca gagcattggc attttccctt tcctgatctt agaagtctga 7980 tgactcatga aaccagacag attagttaca tacaccacaa atcgaggctg tagctggggc 8040 ctcaacactg cagttctttt ataactcctt agtacacttt ttgttgatcc tttgccttga 8100 tccttaattt tcagtgtcta tcacctctcc cgtcagtggt gttccacatt tgggcctatt 8160 ctcagtccag ggagttttac aacaatagat gtattgagaa tccaacctaa agcttaactt 8220 tccactccca tgaatgcctc tctccttttt ctccatttat aaactgagct attaaccatt 8280 aatggttcca ggtggatgtc tcctccccat attacctgat gtatcttaca tattgccagg 8340 ctgatatttt aagacattaa aaggtatatt tcattattga gccacatggt attgattact 8400 gcttactaaa attttgtcat tgtacacatc tgtaaaaggt ggttcctttt ggaatgcaaa 8460 gttcaggtgt ttgttgtctt tcctgaccta aggtcttgtg agcttgtatt ttttctattt 8520 aagcagtgct ttctcttgga ctggcttgac tcatggcatt ctacacgtta ttgctggtct 8580 aaatgtgatt ttgccaagct tcttcaggac ctataatttt gcttgacttg tagccaaaca 8640 caagtaaaat gattaagcaa caaatgtatt tgtgaagctt ggtttttagg ttgttgtgtt 8700 gtgtgtgctt gtgctctata ataatactat ccaggggctg gagaggtggc tcggagttca 8760 agagcacaga ctgctcttcc agaagtcctg agttcaattc ccagcaacca catggtggct 8820 cacaaccatc tgtaatggga tctgatgccc tcttctggtg tgtctgaaga ccacaagtgt 8880 attcacatta aataaataaa tcctccttct tcttcttttt ttttttttta aagagaatac 8940 tgtctccagt agaatttact gaagtaatga aatactttgt gtttgttcca atatggtagc 9000 caataatcaa attactcttt aagcactgga aatgttacca aggaactaat ttttatttga 9060 agtgtaactg tggacagagg agccataact gcagacttgt gggatacaga agaccaatgc 9120 agactttaat gtcttttctc ttacactaag caataaagaa ataaaaattg aacttctagt 9180 atcctatttg tttaaactgc tagctttact taacttttgt gcttcatcta tacaaagctg 9240 aaagctaagt ctgcagccat tactaaacat gaaagcaagt aatgataatt ttggatttca 9300 aaaatgtagg gccagagttt agccagccag tggtggtgct tgcctttatg cctttaatcc 9360 cagcactctg gaggcagaga caggcagatc tctgagtttg agcccagcct ggtctacaca 9420 tcaagttcta tctaggatag ccaggaatac acacagaaac cctgttgggg aggggggctc 9480 tgagatttca taaaattata attgaagcat tccctaatga gccactatgg atgtggctaa 9540 atccgtctac ctttctgatg agatttgggt attatttttt ctgtctctgc tgttggttgg 9600 gtcttttgac actgtgggct ttctttaaag cctccttcct gccatgtggt ctcttgtttg 9660 ctactaactt cccatggctt aaatggcatg gctttttgcc ttctaagggc agctgctgag 9720 atttgcagcc tgatttccag ggtggggttg ggaaatcttt caaacactaa aattgtcctt 9780 taattttttt tttaaaaaat gggttatata ataaacctca taaaatagtt atgaggagtg 9840 aggtggacta atattaaatg agtccctccc ctataaaaga gctattaagg ctttttgtct 9900 tatacttaac ttttttttta aatgtggtat ctttagaacc aagggtctta gagttttagt 9960 atacagaaac tgttgcatcg cttaatcaga ttttctagtt tcaaatccag agaatccaaa 10020 ttcttcacag ccaaagtcaa attaagaatt tctgactttt aatgttaatt tgcttactgt 10080 gaatataaaa atgatagctt ttcctgaggc agggtctcac tatgtatctc tgcctgatct 10140 gcaacaagat atgtagacta aagttctgcc tgcttttgtc tcctgaatac taaggttaaa 10200 atgtagtaat acttttggaa cttgcaggtc agattctttt ataggggaca cactaaggga 10260 gcttgggtga tagttggtaa aatgtgtttc aagtgatgaa aacttgaatt attatcaccg 10320 caacctactt tttaaaaaaa aaagccaggc ctgttagagc atgcttaagg gatccctagg 10380 acttgctgag cacacaagag tagttacttg gcaggctcct ggtgagagca tatttcaaaa 10440 aacaaggcag acaaccaaga aactacagtt aaggttacct gtctttaaac catctgcata 10500 tacacaggga tattaaaata ttccaaataa tatttcattc aagttttccc ccatcaaatt 10560 gggacatgga tttctccggt gaataggcag agttggaaac taaacaaatg ttggttttgt 10620 gatttgtgaa attgttttca agtgatagtt aaagcccatg agatacagaa caaagctgct 10680 atttcgaggt ctcttggttt atactcagaa gcacttcttt gggtttccct gcactatcct 10740 gatcatgtgc taggcctacc ttaggctgat tgttgttcaa ataaacttaa gtttcctgtc 10800 aggtgatgtc atatgatttc atatatcaag gcaaaacatg ttatatatgt taaacatttg 10860 tacttaatgt gaaagttagg tctttgtggg tttgattttt aattttcaaa acctgagcta 10920 aataagtcat ttttacatgt cttacatttg gtggaattgt ataattgtgg tttgcaggca 10980 agactctctg acctagtaac cctacctata gagcactttg ctgggtcaca agtctaggag 11040 tcaagcattt caccttgaag ttgagacgtt ttgttagtgt atactagttt atatgttgga 11100 ggacatgttt atccagaaga tattcaggac tatttttgac tgggctaagg aattgattct 11160 gattagcact gttagtgagc attgagtggc ctttaggctt gaattggagt cacttgtata 11220 tctcaaataa tgctggcctt ttttaaaaag cccttgttct ttatcaccct gttttctaca 11280 taatttttgt tcaaagaaat acttgtttgg atctcctttt gacaacaata gcatgttttc 11340 aagccatatt ttttttcctt tttttttttt tttttggttt ttcgagacag ggtttctctg 11400 tatagccctg gctgtcctgg aactcacttt gtagaccagg ctggcctcga actcagaaat 11460 ccgcctgcct ctgcctcctg agtgccggga ttaaaggcgt gcaccaccac gcctggctaa 11520 gttggatatt ttgttatata actataacca atactaactc cactgggtgg atttttaatt 11580 cagtcagtag tcttaagtgg tctttattgg cccttcatta aaatctactg ttcactctaa 11640 cagaggctgt tggtactagt ggcacttaag caacttccta cggatatact agcagattaa 11700 gggtcaggga tagaaactag tctagcgttt tgtataccta ccagctttat actaccttgt 11760 tctgatagaa atatttcagg acat 11784 21 20 DNA Artificial oligonucleotide 21 gcgtgagatc aagacgcaca 20 22 21 DNA Artificial Oligonucleotide 22 gcagcggtaa gagtccttga t 21 23 19 DNA Artificial Oligonucleotide 23 gtgaacgtgg tgatcaaca 19 24 19 DNA Artificial Oligonucleotide 24 gcagtacagc ttgtccatg 19 25 20 DNA Artificial Oligonucleotide 25 atcctctgca tggtcaggtc 20 26 18 DNA Artificial Oligonucleotide 26 cgtggcctga ttcattcc 18 

What is claimed:
 1. A genetically engineered nucleic acid molecule encoding a phiC31 integrase, wherein the nucleic acid molecule comprises a nucleotide sequence optimized for expression in a eukaryotic host cell, wherein the nucleotide sequence comprises at least 306 codons that are optimal for expression in the eukaryotic host cell, and wherein the phiC31 integrase catalyzes recombination at phiC31 recognition sequences in the eukaryotic host cell.
 2. The nucleic acid molecule of claim 1, wherein the nucleotide sequence comprises at least 430 codons that are optimal for expression in the eukaryotic host cell.
 3. The nucleic acid molecule of claim 1, wherein the nucleotide sequence comprises at least 550 codons that are optimal for expression in the eukaryotic host cell.
 4. The nucleic acid molecule of claim 1 wherein the nucleic acid encodes a protein comprising the amino acid sequence presented in SEQ ID NO:2.
 5. The nucleic acid molecule of claim 1, wherein the eukaryotic host cell is from a species selected from the group consisting of mouse, rat, human, rabbit, and teleost.
 6. The nucleic acid molecule of claim 1, wherein the nucleotide sequence does not contain a splice donor sequence selected from the group consisting of AAGgtaagt, AAGgtgagt, CAGgtaagt, and CAGgtgagt.
 7. The nucleic acid molecule of claim 1, wherein the nucleotide sequence does not contain a splice donor sequence, wherein the splice donor sequence consists of nine contiguous nucleotides, wherein the fourth and fifth positions of the splice donor sequence consist of a G and a T, respectively, and wherein at least five of the nucleotides in the first, second, third, six, seventh, eighth, and ninth positions are identical to the nucleotide in the corresponding position in any one of the sequences selected from the group consisting of AAGgtaagt, AAGgtgagt, CAGgtaagt, CAGgtgagt.
 8. The nucleic acid molecule of claim 1, wherein the nucleotide sequence does not contain a splice donor sequence, wherein the splice donor sequence consists of nine contiguous nucleotides, wherein the fourth and fifth positions of the splice donor sequence consist of a G and a T, respectively, and wherein at least four of the nucleotides in the first, second, third, six, seventh, eighth, and ninth positions are identical to the nucleotide in the corresponding position in any one of the sequences selected from the group consisting of AAGgtaagt, AAGgtgagt, CAGgtaagt, CAGgtgagt.
 9. The nucleic acid molecule of claim 1, wherein the nucleotide sequence does not contain a splice donor sequence, wherein the splice donor sequence consists of nine contiguous nucleotides, wherein the fourth and fifth positions of the splice donor sequence consist of a G and a T, respectively, and wherein at least three of the nucleotides in the first, second, third, six, seventh, eighth, and ninth positions are identical to the nucleotide in the corresponding position in any one of the sequences selected from the group consisting of AAGgtaagt, AAGgtgagt, CAGgtaagt, CAGgtgagt.
 10. The nucleic acid molecule of claim 1, wherein the nucleotide sequence does not contain a splice acceptor sequence, wherein the splice acceptor sequence is selected from the group consisting of SEQ ID NO:3 and SEQ ID NO:4.
 11. The nucleic acid molecule of claim 1, wherein the nucleotide sequence does not contain a splice acceptor sequence, wherein the splice acceptor sequence consists of 12 contiguous nucleotides, wherein the ninth position of the nucleotide sequence of the splice acceptor consists of a C or a T, wherein the tenth and eleventh positions of the nucleotide sequence of the splice acceptor consist an A and a G respectively, and wherein at least five of the nucleotides in the first, second, third, fourth, fifth sixth, seventh, and twelfth positions are identical to the nucleotide in the corresponding position in any one of the sequences presented as SEQ ID NO:3 and SEQ ID NO:4.
 12. The nucleic acid molecule of claim 1, wherein the nucleotide sequence does not contain a splice acceptor sequence, wherein the splice acceptor sequence consists of 12 contiguous nucleotides, wherein the ninth position of the nucleotide sequence of the splice acceptor consists of a C or a T, wherein the tenth and eleventh positions of the nucleotide sequence of the splice acceptor consist an A and a G, respectively, and wherein at least four of the nucleotides in the first, second, third, fourth, fifth sixth, seventh, and twelfth positions are identical to the nucleotide in the corresponding position in any one of the sequences presented as SEQ ID NO:3 and SEQ ID NO:4.
 13. The nucleic acid molecule of claim 1, wherein the nucleotide sequence comprises fewer than 200 CG dinucleotides.
 14. The nucleic acid molecule of claim 13, wherein the nucleotide sequence comprises fewer than 150 CG dinucleotides.
 15. The nucleic acid molecule of claim 13, wherein the nucleotide sequence comprises fewer than 100 CG dinucleotides.
 16. The nucleic acid molecule of claim 13, wherein the nucleotide sequence comprises fewer than 50 CG dinucleotides.
 17. The nucleic acid molecule of claim 13 wherein nucleotide sequence does not comprise the sequence RRCGYY.
 18. The nucleic acid molecule of claim 13 having a coding sequence, wherein the nucleotide sequence does not comprise any CG dinucleotides in its coding sequence.
 19. The nucleic acid molecule of claim 1 that has the sequence presented as SEQ ID NO:5.
 20. The nucleic acid molecule of claim 1 having a translational start codon and a first translational termination codon, which further comprises at least one nucleotide sequence selected from the group consisting of: a) a Kozak consensus sequence that spans the translational start codon, b) a nucleotide sequence 3′ of the phiC31 integrase encoding region, which encodes a nuclear localization signal, and c) a second translational termination codon positioned immediately 3′ to the first translational termination codon.
 21. The nucleic acid molecule of claim 20 that has the sequence presented as SEQ ID NO:8 or SEQ ID NO:13.
 22. The phiC31 integrase encoded by the nucleic acid molecule or any of claims 1, 6, 10, 13, 17, or
 20. 23. A DNA vector comprising the nucleic acid presented in any of claims 1, 6, 10, 13, 17, or
 20. 24. A microorganism comprising the vector on claim
 23. 25. A vertebrate cell comprising in its genome the nucleic acid presented in any of claims 1, 6, 10, 13, 17, or
 20. 26. The vertebrate cell of claim 25 that further comprises in its genome phiC31 integrase recognition sequences.
 27. A transgenic organism that comprises in its genome the nucleic acid presented in any of claims 1, 6, 10, 13, 17, or
 20. 28. A transgenic organism according to claim 27 that further comprises in its genome phiC31 integrase recognition sequences.
 29. A method of recombining a DNA molecule containing phiC31 integrase recognition sequences in a eukaryotic cell, said method comprising contacting the cell with a phiC31 integrase according to any of claims 1, 6, 10, 13, 17, or 20, wherein the phiC31 integrase catalyzes recombination of the DNA molecule. 